Microorganisms; General Exemptions From Reporting Requirements; Revisions to Recipient Organisms Eligible for Tier I and Tier II Exemptions, 13760-13773 [2020-04746]
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Federal Register / Vol. 85, No. 47 / Tuesday, March 10, 2020 / Rules and Regulations
ENVIRONMENTAL PROTECTION
AGENCY
40 CFR Part 725
[EPA–HQ–OPPT–2011–0740; FRL–9991–60]
RIN 2070–AJ65
Microorganisms; General Exemptions
From Reporting Requirements;
Revisions to Recipient Organisms
Eligible for Tier I and Tier II
Exemptions
Environmental Protection
Agency (EPA).
ACTION: Final rule.
AGENCY:
EPA is issuing a final rule to
add Trichoderma reesei (T. reesei) strain
QM6a and its derivatives and Bacillus
amyloliquefaciens (B.
amyloliquefaciens) subspecies (subsp.)
amyloliquefaciens to the list of recipient
microorganisms that may be used to
qualify for the Tier I and Tier II
exemptions from full notification and
reporting procedures under the Toxic
Substances Control Act (TSCA) for new
microorganisms that are being
manufactured for introduction into
commerce. EPA received petitions to
add T. reesei and B. amyloliquefaciens
to the list of microorganisms eligible for
the exemption from full notification and
reporting procedures under the TSCA
for new microorganisms. Based on
EPA’s evaluation of these petitions, EPA
has made the determination that certain
strains of both microorganisms will not
present an unreasonable risk of injury to
health or the environment when used as
a recipient microorganism provided that
certain criteria for the introduced
genetic material and the physical
containment conditions are met.
DATES: This final rule is effective April
9, 2020.
ADDRESSES: The docket for this action,
identified by docket identification (ID)
number EPA–HQ–OPPT–2011–0740, is
available at https://www.regulations.gov
or at the Office of Pollution Prevention
and Toxics Docket (OPPT Docket),
Environmental Protection Agency
Docket Center (EPA/DC), West William
Jefferson Clinton Bldg., Rm. 3334, 1301
Constitution Ave. NW, Washington, DC.
The Public Reading Room is open from
8:30 a.m. to 4:30 p.m., Monday through
Friday, excluding legal holidays. The
telephone number for the Public
Reading Room is (202) 566–1744, and
the telephone number for the OPPT
Docket is (202) 566–0280. Please review
the visitor instructions and additional
information about the docket available
at https://www.epa.gov/dockets.
FOR FURTHER INFORMATION CONTACT:
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SUMMARY:
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For technical information contact:
Rebecca Edelstein, Chemical Control
Division (7405M), Office of Pollution
Prevention and Toxics, Environmental
Protection Agency, 1200 Pennsylvania
Ave. NW, Washington, DC 20460–0001;
telephone number: (202) 564–1667;
email address: edelstein.rebecca@
epa.gov.
For general information contact: The
TSCA-Hotline, ABVI-Goodwill, 422
South Clinton Ave., Rochester, NY
14620; telephone number: (202) 554–
1404; email address: TSCA-Hotline@
epa.gov.
SUPPLEMENTARY INFORMATION:
I. Executive Summary
A. Does this action apply to me?
You may be potentially affected by
this action if you produce, import,
process, or use either intergeneric T.
reesei or intergeneric B.
amyloliquefaciens or any other eligible
recipient microorganisms listed in 40
CFR 725.420. The following list of North
American Industrial Classification
System (NAICS) codes is not intended
to be exhaustive, but rather provides a
guide to help readers determine whether
this document applies to them.
Potentially affected entities may
include:
• Basic Chemical Manufacturing
(NAICS code 3251).
• Pesticide, Fertilizer and other
Agricultural Chemical manufacturing
(NAICS code 3253).
• Other Chemical Product and
Preparation Manufacturing (NAICS code
3259).
If you have any questions regarding
the applicability of this action to a
particular entity, consult the technical
person listed under FOR FURTHER
INFORMATION CONTACT.
B. What is the Agency’s authority for
taking this action?
This action is being taken under the
authority of TSCA section 5(h)(4) (15
U.S.C. 2604(h)(4)). TSCA section 5(a)(1)
requires that persons notify EPA at least
90 days before they manufacture (the
term ‘‘manufacture’’ includes import
under TSCA) for commercial purposes a
‘‘new’’ chemical substance, or
manufacture (including import) or
process a chemical substance for a
‘‘significant new use’’ (15 U.S.C.
2604(a)(1)(B)(i)). TSCA furthermore
prohibits such manufacturing or
processing from commencing until EPA
has conducted a review of the notice,
made an appropriate determination on
the notice, and taken such actions as are
required in association with that
determination (15 U.S.C.
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2604(a)(1)(B)(ii)). TSCA defines
‘‘chemical substance’’ broadly and in
terms that cover intergeneric
microorganisms as well as traditional
chemical substances. Therefore, for the
purposes of TSCA, a ‘‘new
microorganism’’ is one that is not listed
on the TSCA Chemical Substances
Inventory (TSCA Inventory) compiled
under TSCA section 8(b).
TSCA section 5(h)(4) authorizes EPA,
upon application and by rule, to exempt
the manufacturer of any new chemical
substance from part or all of the
provisions of TSCA section 5, if EPA
determines that the manufacture,
processing, distribution in commerce,
use, or disposal of the new chemical
substance will not present an
unreasonable risk of injury to human
health or the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation
identified by the Administrator under
the conditions of use.
C. What action is the Agency taking?
In 2012, EPA proposed to add T.
reesei strain QM6a and its derivatives
(hereafter, T. reesei QM6a) and B.
amyloliquefaciens subspecies (subsp.)
amyloliquefaciens to the list of recipient
microorganisms in 40 CFR 725.420 that
may be used to qualify for Tier I and
Tier II exemptions from full notification
and reporting procedures under TSCA
for new microorganisms that are being
manufactured into commerce. EPA is
finalizing the proposal.
D. Why is the Agency taking this action?
EPA received petitions to add T.
reesei and B. amyloliquefaciens to the
list of microorganisms that may be used
as recipient microorganisms in order to
qualify for the exemption from full
notification and reporting procedures
under TSCA for new microorganisms
that are being manufactured for
introduction into commerce. EPA
proposed to add certain strains of these
two microorganisms to the list of
recipient microorganisms based on
EPA’s preliminary determination. EPA
is now issuing a final rule that
incorporates certain changes in response
to public comment.
E. What are the estimated incremental
impacts of this final rule?
EPA has evaluated the potential costs
of the addition of the two
microorganisms to the list of recipient
microorganisms eligible for Tier I and
Tier II exemptions. The final rule is
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expected to generate cost savings for
organizations that, in the absence of the
rule, would submit Microbial
Commercial Activity Notices (MCANs)
for new intergeneric T. reesei or B.
amyloliquefaciens strains. The rule will
result in costs savings for both the
industry and the Agency. EPA estimates
the annualized industry savings of the
rule to be approximately $260,000 per
year over a ten-year period, with a 3
percent discount rate, and $252,000 per
year with a 7 percent discount rate.
Annualized agency savings are
approximately $178,000 per year with a
3 percent discount rate and $173,000
per year with a 7 percent discount rate
over the ten-year period, for a total
annualized savings to society of
approximately $438,000 per year with a
3 percent discount rate and $424,000
per year with a 7 percent discount rate.
The economic analysis is available in
the docket and is summarized in Unit
IX. of this final rule. Costs and benefits
of adding T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens to 40 CFR 725.420
are also discussed in Unit VIII.C.2.
through 4.
II. Background
EPA received petitions to add T.
reesei and B. amyloliquefaciens to the
list of recipient microorganisms at 40
CFR 725.420 that are eligible for the
regulatory exemptions applicable to
new microorganisms that are
manufactured for introduction into
commerce (Refs. 1–3). In the Federal
Register of September 5, 2012 (77 FR
54499) (FRL–9348–1) (‘‘2012 Proposed
Rule’’) (Ref. 4), the Agency proposed to
add certain strains of these two
microorganisms to the list of recipient
microorganisms at 40 CFR 725.420
based on EPA’s preliminary
determination that both of the
microorganisms, with certain
limitations, meet the criteria for
addition to the list—i.e., they will not
present an unreasonable risk of injury to
health or the environment provided that
the other conditions of the exemptions
at 40 CFR part 725, subpart G, relating
to the introduced genetic material, and
the physical containment of the new
microorganisms, have been met. EPA is
now issuing a final rule that
incorporates certain changes made in
response to public comments received
on the 2012 Proposed Rule. These
changes are described in the following
paragraphs.
In the 2012 Proposed Rule, EPA
proposed to restrict the exemption for T.
reesei to the T. reesei strain QM6a and
its derivatives. In addition, EPA
proposed to restrict the T. reesei QM6a
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exemption to use of the microorganism
only under submerged standard
industrial fermentation operations used
for enzyme production; as described in
this proposed rule, these conditions are
typical throughout the fermentation
industry and meet the existing physical
containment and control requirements
for the tiered exemptions under 40 CFR
725.422. Any subsequent deliberate
fermentation of solid plant material or
insoluble substrates with T. reesei
QM6a and its derivatives as defined at
40 CFR 725.3 could only be initiated
after inactivation of the viable T. reesei
cells as delineated in 40 CFR
725.422(d), i.e., by a procedure that has
been demonstrated and documented to
be effective in reducing the viable
microbial population by at least 6 logs
(i.e., six orders of magnitude).
In addition, EPA proposed to limit the
exemption for B. amyloliquefaciens to
only strains of B. amyloliquefaciens that
would fall under the subspecies B.
amyloliquefaciens amyloliquefaciens.
In response to comments received on
its original proposal, EPA has modified
the regulatory text in 40 CFR 725.3 and
725.420 slightly to better clarify EPA’s
original intent. These revisions to the
regulatory text in 40 CFR 725.3 and
725.420 merely represent a clarification
of the original proposal.
Existing regulatory requirements and
exemptions for intergeneric
microorganisms are discussed in Unit
III. of this proposed rule. EPA’s
response to public comments received
on the 2012 Proposed Rule are provided
in Unit IV. Unit V. provides EPA’s
evaluation of available information on
T. reesei and B. amyloliquefaciens for
the criteria delineated in 40 CFR 725.67.
Physical containment and control
technologies as well as release and
exposure assessments for the two
microorganisms are discussed in Unit
VI. EPA’s risk assessments for T. reesei
QM6a and B. amyloliquefaciens subsp.
amyloliquefaciens are summarized in
Unit VII., and EPA’s rationale for adding
the two microorganisms to the list of
recipients eligible for exemption is
discussed in Unit VIII. EPA’s Risk
Assessment documents (Refs. 5 and 6),
available in the public docket, provide
more detailed information, and
supporting references, for EPA’s
evaluation of the available information
and the potential risks to health and the
environment.
III. Existing EPA Regulatory
Requirements and Exemption Standard
Manufacturers are required to report
certain information to EPA 90 days
before commencing the manufacture of
intergeneric microorganisms that are not
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listed on the TSCA Inventory. EPA
regulations at 40 CFR part 725 establish
the mechanisms for reporting this
information. TSCA prohibits such
manufacturing or processing from
commencing until EPA has conducted a
review of the notice, made an
appropriate determination on the notice,
and taken such actions as are required
in association with that determination
(15 U.S.C. 2604(a)(1)(B)(ii)).
Any manufacturer of a living
intergeneric microorganism who is
required to report under TSCA section
5 must file a MCAN with EPA, unless
the activity is eligible for one of the
specific exemptions. Section 5(h)(4)
authorizes EPA, by rule and upon
request, to exempt manufacturers from
these requirements if the Administrator
determines that the manufacture,
processing, distribution in commerce,
use or disposal of the chemical
substance ‘‘will not present an
unreasonable risk of injury to health or
the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation
identified by the Administrator under
the conditions of use.’’ TSCA section
3(4) defines ‘‘conditions of use’’ to mean
‘‘the circumstances, as determined by
the Administrator, under which a
chemical substance is intended, known
or reasonably foreseen to be
manufactured, processed, distributed in
commerce, used, or disposed of.’’ TSCA
section 3(12) defines ‘‘potentially
exposed or susceptible subpopulation’’
to mean ‘‘a group of individuals within
the general population. . .who, due to
either greater susceptibility or greater
exposure, may be at greater risk than the
general population of adverse health
effects from exposure to a chemical
substance or mixture, such as infants,
children, pregnant women, workers, or
the elderly.’’ 15 U.S.C. 2601 et seq. The
general procedures for filing MCANs are
described in 40 CFR part 725, subpart B.
EPA regulations establish two
exemptions for new microorganisms,
after the research and development
stage, which are being manufactured for
introduction into commerce: Tier I and
Tier II exemptions.
Under the Tier I exemption, if certain
criteria are met, manufacturers are
required to notify EPA 10 days prior to
manufacturing a new microorganism
that qualifies for this exemption, and to
keep certain records. 40 CFR 725.400.
To qualify for the Tier I exemption, a
manufacturer must use one of the
recipient organisms listed in 40 CFR
725.420, and must implement specific
physical containment and control
technologies listed in 40 CFR 725.422.
In addition, the genetic material
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introduced into the recipient
microorganism must be wellcharacterized, limited in size, poorly
mobilizable, and free of certain
sequences. 40 CFR 725.421.
A manufacturer who meets the
conditions of the Tier I exemption may
modify the specified containment
restrictions or level of inactivation but
must submit a Tier II exemption
notification 40 CFR 725.428. The Tier II
exemption requires manufacturers to
submit an abbreviated notification
describing the modified containment
and provides for a 45-day period during
which EPA would review the proposed
containment. 40 CFR 725.450 and
725.470. The manufacturer may not
proceed under this exemption until EPA
approves the exemption. 40 CFR
725.470.
EPA established a petition process at
40 CFR 725.67 for the public to propose
additional microorganisms for the tiered
exemptions. EPA’s regulations at 40
CFR 725.67 direct petitioners to submit
information to demonstrate that the
activities affected by the requested
exemption meet the requirements of
TSCA section 5(h)(4), i.e. ‘‘will not
present an unreasonable risk of injury to
health or the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation
identified by the Administrator under
the conditions of use.’’ 15 U.S.C.
2604(h)(4). In addition, a petitioner is
responsible for providing supporting
information for this determination in
four general categories:
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1. The effects of the new microorganism on
health and the environment.
2. The magnitude of exposure of human
beings and the environment to the new
microorganism.
3. The benefits of the new microorganism
for various uses and the availability of
substitutes for such uses.
4. The reasonably ascertainable economic
consequences of granting or denying the
petition, including effects on the national
economy, small business, and technological
innovation.
The regulations at 40 CFR 725.67
specify that when applying to list a
recipient microorganism for the tiered
exemption under 40 CFR 725.420,
petitioners should include information
addressing six specified criteria, which
EPA will use to evaluate the
microorganism for listing. 40 CFR
725.67(a)(3)(iii). The six criteria are:
1. Identification and classification of the
microorganism using available genotypic and
phenotypic information.
2. Information to evaluate the relationship
of the microorganism to any other closely
related microorganisms which have a
potential for adverse effects on health or the
environment.
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3. A history of safe commercial use for the
microorganism.
4. Commercial uses indicating that the
microorganism products might be subject to
TSCA.
5. Studies which indicate the potential for
the microorganism to cause adverse effects to
health or the environment.
6. Studies which indicate the survival
characteristics of the microorganism in the
environment.
IV. Response to Public Comments on
the 2012 Proposed Rule
The Agency received three comments
on the 2012 Proposed Rule (Ref. 4). One
comment, from an anonymous submitter
(Ref. 7), concerned mold problems in
rental housing and thus was not
relevant to the proposed rule. A second
comment, from an individual (Ref. 8),
supported the proposed rule.
The third comment was a joint set of
comments from the Biotechnology
Industry Organization (BIO) and the
Enzyme Technical Association (ETA)
(Ref. 9). While generally supportive of
the proposed rule, BIO/ETA raised three
important issues with respect to EPA’s
proposed rule.
First, BIO/ETA expressed concern
that the proposed wording in section
725.420(k), that reads ‘‘Trichoderma
reesei strain QM6a used only in . . .’’
does not accurately reflect the range of
T. reesei strain QM6a microorganisms
currently being used in standard
industrial fermentations. BIO/ETA
requested that the phrase be reworded
as ‘‘Trichoderma reesei strain QM6a and
its derivatives used only in . . .’’ EPA
agrees that the commenter’s suggested
language more accurately reflects the
Agency’s original intent. EPA did not
originally intend to restrict the
exemption to the naturally occurring
QM6a isolate. Most of the strains of T.
reesei currently used in industrial
production are not the naturally
occurring QM6a isolate, but are strains
derived from QM6a that have been
modified by physical or chemical
mutagenesis to obtain microorganisms
with improved enzyme-producing
abilities. Accordingly, EPA has adopted
the commenter’s suggested revision to
clarify that the exemption applies not
only to the naturally occurring strain,
but also to any strain derived from the
naturally occurring QM6a.
Second, BIO/ETA expressed concern
that the proposed regulation was too
broadly worded and as drafted would
not clearly distinguish between
standard industrial fermentation
operations used to produce enzymes,
and fermentation operations conducted
for other purposes. Specifically, the
commenter raised concern that the
inclusion of an unqualified restriction
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in proposed 40 CFR 725.420(k) that ‘‘no
solid plant material or insoluble
substrate is present in the fermentation
broth’’ would prohibit the use of T.
reesei in submerged standard industrial
fermentation operations used for
enzyme production. Enzyme production
is the first phase of some industrial
applications such as cellulosic ethanol
production where the first fermentation
is to grow the microorganism to produce
enzymes, followed by another
fermentation of pretreated plant biomass
for conversion of the cellulose and
hemicellulose to simple sugars (i.e.,
saccharification), followed by a third
fermentation of the sugars to ethanol by
yeast or another ethanologen. As part of
the process of growing the microbes for
enzyme production by T. reesei QM6a
and its derivatives, nutrients need to be
available, including those from plant
materials such as soy or corn, which
may contain insoluble components. The
second fermentation operation of
saccharification of plant biomass may
occur only after the T. reesei
microorganism has been inactivated.
The use of nutrients supplied by plant
material (e.g., soy meal, corn steep
liquor) in the first fermentation for
enzyme production has a long history of
safe use.
To address this issue, the commenter
suggested revising the regulatory text to
ensure that the typical industry practice
of supplying nutrients in the form of
solid plant materials during the initial
enzyme fermentation would fall within
the scope of the proposed exemption.
EPA agrees and is therefore changing
the regulatory text to allow the use of
solid plant material in the enzyme
fermentation step. Under the final
regulatory text, the use of the
conventional fermentation ingredients
from solid plant material—for example,
soy or corn meal and other insoluble
fermentation ingredients from corn or
soy which contain insoluble
components—is allowed when used
specifically to provide nutrients for
growth of the microorganism during
standard enzyme fermentation as
described in part 1 of the definition at
40 CFR 725.3.
The commenter further suggested
adding text to clarify that the
requirement to inactivate the organism
applies prior to ‘‘subsequent
fermentation operations, and not to the
initial enzyme production stage.’’ EPA
agrees that the commenter has identified
a reasonable basis for concern with
respect to the proposed regulatory text.
EPA acknowledges that nutrients for
microbial growth in submerged standard
industrial fermentation during the
initial enzyme production phase of the
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fermentation operation may be supplied
by soybean meal, corn steep liquor, or
other plant-derived materials that may
contain insoluble substrates. The use of
such plant materials as nutrient sources
for microbial growth in submerged
standard industrial fermentation
operations used for enzyme production
is a standard industry practice with a
long history of safe use, and it does not
result in the production of secondary
toxic metabolites such as paracelsin
because the fermentations involve the
logarithmic growth of the cells in the
presence of optimal concentrations of
carbon and nitrogen and other nutrients
(see Unit V. for more detail on
paracelsin). EPA did not originally
intend to preclude such operations and
agrees that revision to the regulatory
text is warranted to clarify that solid
plant material can be used to provide
nutrients for growth of the
microorganism during submerged
standard enzyme fermentation
operations.
However, EPA continues to have
concern about the potential for the
production of paracelsin during the
second fermentation phase of cellulosic
ethanol production, i.e., the
saccharification of the pretreated plant
biomass, because of the presence of
solid surfaces and an excess of carbon
substrate with live T. reesei QM6a (and
its derivatives) cells. Therefore, EPA is
retaining the requirement that
fermentation operations subsequent to
the enzyme production fermentation
phase may only be initiated after
inactivation of the viable T. reesei cells
as delineated in 40 CFR 725.422(d) (i.e.,
by a procedure that has been
demonstrated and documented to be
effective in reducing the viable
microbial population by at least 6 logs).
Inactivation of T. reesei QM6a prior to
a subsequent or secondary fermentation
that may contain solid plant material or
insoluble substrates (as defined at 40
CFR 725.3) avoids the potential for
production of paracelsin.
BIO/ETA also commented that
paracelsin may be produced under nonstandard conditions of fermentation,
such as ‘‘surface fermentation media
with large concentrations of biomass,’’
and requested that EPA revise the rule
to reflect this. EPA interprets this
comment to mean ‘‘surface fermentation
media with large concentrations of
biomass’’ is the only condition under
which paracelsin can be produced and
that BIO/ETA is requesting that the rule
be amended accordingly. EPA agrees
that paracelsin may be produced under
non-standard conditions of
fermentation, such as surface
fermentation with large concentrations
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of biomass. However, available
scientific literature indicates that
paracelsin may also be produced under
certain other fermentation conditions.
Scientific literature suggests that surface
fermentation is synonymous with solidstate fermentation where
microorganisms are grown on the
surface of a solid support that is not
submerged. While it is likely that the
potential for paracelsin production is
greater with solid-state/surface
fermentation, the production of
peptaibols (of which paracelsin is one)
by Trichoderma species has been shown
to occur even in liquid broth culture in
the presence of plant material or
insoluble substrates in laboratory
studies. Thus, paracelsin production
potentially may be produced in
fermentation broth amended with plant
material providing excess carbon.
Therefore, EPA is not amending the rule
to indicate that the only conditions in
which paracelsin potentially may be
produced are with surface fermentations
with large concentrations of biomass.
provided that: (a) The existing criteria
for the introduced genetic material
listed in 40 CFR 725.422 are met, and
(b) the physical containment and
control technologies criteria listed at 40
CFR 725.422 are met. In making this
determination, EPA identified workers
as a potentially exposed or susceptible
subpopulation to the substances under
the conditions of use and concluded
that, with the limitations described
above, the substances will not present
an unreasonable risk of injury to health
or the environment. EPA’s Risk
Assessments for these two
microorganisms (Refs. 5 and 6) are
available in the docket.
This unit presents a summary of
EPA’s evaluation of the available
information pertinent to the six criteria
delineated in 40 CFR 725.67(a)(3)(iii) for
both microorganisms.
V. EPA’s Evaluation of Available
Information on T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens for the Criteria
Delineated
Pursuant to 40 CFR 725.67, Genencor
International, Inc., (subsequently
supported by the Enzyme Technical
Association (ETA)) and Novozymes
North America, Inc., submitted Letters
of Application to EPA requesting that T.
reesei and B. amyloliquefaciens (Refs. 1
and 2) be added to 40 CFR 725.420 as
candidate recipient microorganisms for
the tiered exemptions. The letters of
application provided information that
the submitters believed demonstrate
that activities affected by the requested
exemptions would not present an
unreasonable risk of injury to health or
the environment. Information regarding
the criteria specified in 40 CFR
725.67(a)(2) and 725.67(a)(3)(iii) were
addressed in these letters of application
to list T. reesei and B. amyloliquefaciens
as recipient microorganisms under 40
CFR 725.420.
EPA has made the determination
based on the information provided in
the Letters of Application (Refs. 1 and
2), supplemental information provided
by ETA (Refs. 10 and 11), and other
information available to EPA that T.
reesei QM6a, with certain restrictions,
and B. amyloliquefaciens subsp.
amyloliquefaciens will not present an
unreasonable risk of injury to health or
the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation,
when used as recipient microorganisms
1. Identification and classification of
the microorganism using available
genotypic and phenotypic information.
T. reesei is a hypercellulolytic fungus
originally isolated in the Solomon
Islands in 1944. T. reesei was found on
deteriorating military fabrics such as
tents and clothing. This isolate,
designated as QM6a, was initially
named Trichoderma viride.
Approximately 20 years later, QM6a
was re-classified as Trichoderma reesei.
T. reesei is the species name given to
the anamorphic form (this form
reproduces asexually) of the fungus
whose teleomorphic form (this form
reproduces sexually) is now understood
to be Hypocrea jecorina.
Recent taxonomic studies have shown
that the species T. reesei consists only
of this single isolate QM6a and its
derivatives. Many other strains called T.
reesei isolated elsewhere have now been
proposed as belonging to a newly
named species, T. parareesei, based on
differences in habitat, sporulation, and
metabolic versatility. T. reesei has been
shown to belong to a single species now
referred to as H. jecorina/T. reesei
(QM6a) which reflects its relationship to
its teleomorph H. jecorina. The only
anamorphic strains within the species
H. jecorina/T. reesei are those of QM6a
and its derivatives. The petition to add
T. reesei to the list of microorganisms at
40 CFR 725.420 requested that EPA
include all strains of T. reesei. However,
given these recent taxonomic
publications, all fungal strains correctly
named T. reesei are, by definition,
QM6a or a derivative.
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A. Evaluation of Available Information
Relevant to the Criteria for T. reesei
QM6a as a Recipient Microorganism
with Specified Conditions of Growth
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Adequate genotypic and phenotypic
information is available for
classification of T. reesei QM6a and its
derivatives. The American Type Culture
Collection (ATCC) designation for this
original strain of T. reesei QM6a is
ATCC 13631.
2. Information to evaluate the
relationship of the microorganism to
any other closely related
microorganisms that have a potential
for adverse effects on health or the
environment.
Closely related members of section
Longibrachiatum do not have a potential
for adverse effects; other less closely
related Trichoderma species have a
potential to cause adverse effects as
pathogens of commercially produced
mushrooms. These less closely related
species include various species of the
Harzianum clade, T. aggressivum, T.
pleuotrophilum, and T. fulvidum that
are responsible for significant loss of the
mushroom crops of Agaricus bisporus
and Pleurotus ostreatus.
T. reesei/H. jecorina can be
distinguished from other Trichoderma
species by a comprehensive approach
employing criteria of the Genealogical
Concordance Phylogenetic Species
Recognition (GCPSR) concept, which
commonly requires the use of
genealogies of three or four genes, not
just the sequences of spacer regions as
previously utilized for identification.
Use of the GCPSR protocol would
separate T. reesei (sensu lato) from the
opportunistic pathogens within the
section Longibrachiatum, including T.
longibrachiatum and T. citrinoviride/H.
schweinitzii, as well as the mold disease
pathogens of mushrooms.
3. A history of safe commercial use for
the microorganism.
T. reesei QM6a has a long history of
safe use producing a variety of
commercial enzymes. T. reesei QM6a
cellulases, beta-glucanases, and
xylanases are used by the animal feed,
baking, beverages, textile processing,
detergent, pulp and paper, industrial
chemicals, and biofuels industries.
For industrial enzyme production, T.
reesei is generally grown in a closed,
submerged standard industrial
fermentation system. In submerged
standard industrial fermentation
operations used for enzyme production,
growth of the microorganism occurs
beneath the surface of the liquid growth
medium. As described in this unit, this
type of fermentation system appears to
be typical throughout the industry,
based on EPA’s review of MCAN
submissions over the years.
Under this type of fermentation
system, the fermentation broth is a
defined mixture of carbon and nitrogen
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sources, some of which may be supplied
from plant material or soluble substrates
(e.g., soy meal, corn steep liquor),
minerals, salts, and other nutrients, is
maintained at optimal pH and
temperature, and is typically aerated
and mixed. These conditions support
the active growth and productivity of
the organisms for enzyme production.
Submerged standard industrial
fermentation operations used for
enzyme production systems reduce the
potential for exposure of workers to the
production organism and fermentation
broth aerosols, reduce the potential for
contamination of the culture and make
the collection of extracellular enzymes
simpler and less costly. The
fermentation process is terminated
before the T. reesei QM6a organisms go
into the stationary growth phase (i.e.,
before secondary metabolism begins). At
the end of the fermentation process, the
production organisms are separated
from the fermentation broth and
inactivated.
Several enzymes produced by T.
reesei QM6a have Generally Recognized
as Safe (GRAS) status with the Food and
Drug Administration (FDA) or FDA had
no questions about the GRAS
conclusions about them contained in
GRAS submissions to FDA. This
supports the Agency’s conclusion that
commercial use of T. reesei QM6a and
its derivatives as a recipient
microorganism for commercial enzyme
production will not present an
unreasonable risk of injury to health or
the environment. T. reesei QM6a
enzymes used in foods that have been
granted GRAS status or for whose
claimed GRAS status FDA had no
questions include cellulase,
hemicellulase, transglucosidase, pectin
lyase, acid fungal protease, and a
chymosin enzyme preparation. Data
supporting the GRAS notices included
the results of pathogenicity tests for the
T. reesei QM6a production organisms
and toxicity tests for the enzyme
products. The data showed that the
production strains are not pathogenic
and did not produce toxins during
enzyme fermentation.
4. Commercial uses indicating that
the microorganism products might be
subject to TSCA.
EPA has reviewed 48 MCANs
involving intergeneric T. reesei
production organisms used to
manufacture a number of industrial
enzymes, including amylases,
glucosidases, proteases, phytase,
laccase, and numerous cellulolytic
enzyme preparations. Amylases and
glucosidases are used for the breakdown
of starch into sugars and have been used
in laundry detergents and in textile
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processing. More recently, industrial
enzymes produced by T. reesei have
been produced for corn and cellulosic
ethanol production. T. reesei produces
numerous cellulases and hemicellulases
that are efficient in degrading plant
biomass. Intergeneric T. reesei strains
could also be used to manufacture
industrial chemicals other than enzymes
such as surfactants or specialty
chemicals. More detailed information
on MCANs submitted to EPA can be
viewed on EPA’s TSCA Biotechnology
Program web page: https://
www.epa.gov/regulation-biotechnologyunder-tsca-and-fifra/overviewbiotechnology-under-tsca.
5. Studies which indicate the
potential for the microorganism to cause
adverse effects to health or the
environment.
a. Human health hazards — i.
Pathogenicity. T. reesei QM6a is not
pathogenic to humans. Due to its long
history of use for production of enzymes
used in food applications, the potential
for the fungus and its products to be
pathogenic or toxic to humans has been
evaluated numerous times. Various
studies have been conducted assessing
T. reesei QM6a’s pathogenic potential in
healthy and immunocompromised
laboratory animals. With the exception
of one study where a high inoculum of
intravenous (iv) and intraperitoneal (ip)
injection of spores in
immunocompromised mice resulted in
pathogenic effects, studies have
demonstrated a lack of pathogenicity of
T. reesei QM6a. Numerous
pathogenicity studies have been
conducted as part of GRAS notices to
FDA for several different enzymes used
in the food industry. Studies using
injection of T. reesei QM6a in rats, using
both healthy and immunosuppressed
rats, and using ip injection of viable and
heat-killed cells of T. reesei QM6a in
rats have all demonstrated a lack of
potential pathogenicity to humans.
T. reesei QM6A is not known to
possess any virulence factors associated
with colonization or disease such as
adherence factors, penetration factors,
necrotic factors, toxins, or the ability to
grow at human body temperature, 37 °C.
There are no reports of harmful effects
associated with the use of or exposure
to T. reesei QM6A strains, even after
decades of commercial use for enzyme
production. The body of evidence
indicates that T. reesei QM6A does not
pose concerns regarding human
pathogenicity.
ii. Toxicity. Available data indicate
that T. reesei QM6a strains used in
submerged standard industrial
fermentation operations used for
enzyme production do not present
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human toxicity concerns. A number of
studies have been conducted assessing
the potential for T. reesei QM6a to
produce toxins during submerged
standard industrial fermentation
operations used for enzyme production
for food, pharmaceutical, or industrial
uses. A cellulase enzyme known as
celluclast produced by T. reesei QM6a
has been tested for general oral toxicity
and inhalation toxicity. Acute oral
toxicity studies conducted in mice, rats,
and dogs showed that T. reesei QM6a
cellulase was not toxic to any of the test
animals. Subchronic toxicity studies
showed no evidence of systemic effects
in dogs or rats. Additional toxicity
studies have been conducted on other
enzymes produced by T. reesei QM6a,
the results of which have been
presented in various GRAS petitions.
Acute oral toxicity tests on two
endoglucanases and a glucoamylase
showed a lack of toxins. Subchronic
feeding studies conducted on a
cellulase, two xylanases, two
endoglucanases, a protease, and a
glucoamylase also showed a lack of
toxicity in rats.
Under typical industry practice,
industrial fermentations of T. reesei
QM6a for enzymes to be used in food
are routinely checked by the enzyme
producers to confirm the absence of
antibiotic activity and toxins (Ref. 12).
Relying on the data that show T. reesei
QM6a has a long history of safe use in
the production of food enzymes, EPA
has concluded that strains used
industrially would not be expected to
produce these toxins under the
conditions of submerged standard
industrial fermentation used for enzyme
production.
iii. Mycotoxins and other secondary
metabolites. The only health concern
associated with T. reesei QM6a is its
ability to produce a peptaibol secondary
metabolite called paracelsin. Peptaibols
are small linear peptides of 1,000–2,000
daltons characterized by a high content
of the non-proteinogenic amino acid aamino-isobutyric acid (Aib), with an Nterminus that is typically acetylated,
and a C-terminus that is linked to an
amino alcohol, which is usually
phenylalaninol, or sometimes valinol,
leucinol, isoleucinol, or tryptophanol.
Peptaibols are associated with a wide
variety of biological activities and have
antifungal, antibacterial, sometimes
antiviral, antiparasitic, and neurotoxic
activity. Paracelsin has been shown to
damage mammalian cells such as
human erythrocytes with an in vitro
hemolytic activity of C50 = 3.7 x 10 5
mole/liter (mol/L) (Ref. 5).
Paracelsin has not been detected in
the use of T. reesei QM6a under the
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submerged standard industrial
fermentation operations used for
enzyme production, and numerous
toxicity studies on enzyme products of
T. reesei QM6a have demonstrated a
lack of toxicity to laboratory animals.
EPA therefore expects that paracelsin
production would be of insignificant
concern, provided the microorganisms
are produced with submerged standard
industrial fermentation operations used
for enzyme production as described at
40 CFR 725.3.
Under other conditions of
fermentation, for example with the
deliberate fermentation of cellulosic
biomass for saccharification of plant
material or extended fermentation,
paracelsin may be produced (Ref. 5).
Neither the information submitted with
the petition, nor the information that is
otherwise available is sufficient to allow
EPA to determine the extent of
paracelsin formation under these nonstandard conditions. Consequently, EPA
is unable to determine whether the use
of the microbe under conditions other
than submerged standard industrial
fermentation operations used for
enzyme production (i.e., specific
conditions under which paracelsin is
not expected to be formed) will not pose
an unreasonable risk to human health
and/or the environment (Ref. 5).
b. Environmental hazards—i. Hazards
to animals. T. reesei QM6a is not
pathogenic to domesticated animals or
wildlife. However, the secondary
metabolite paracelsin has been shown to
exhibit toxicity to aquatic species. A 24hr exposure of paracelsin to Artemia
salina (brine shrimp) resulted in a lethal
concentration of 50% (LC50) of 21.26
micromoles (mM) (40.84 micrograms per
milliliter (mg/ml)) which decreased to
9.66 mM (18.56 mg/ml) with a 36-hr
exposure. With Daphnia magna,
paracelsin was found to be moderately
toxic, with an LC50 of 7.70 mM (14.79 mg/
ml) with a 24-hr exposure, and 5.60 mM
(10.76 mg/ml) with a 36-hr exposure.
ii. Hazards to plants. T. reesei QM6a
is not a pathogen of plants. Although it
is capable of degrading cellulose and
hemicellulose due to the copious
quantities of the enzymes it can
produce, it cannot be a primary
colonizer on plant tissue. Genetic
studies have shown that T. reesei QM6a
does not contain any genes for
ligninases, required for initial
breakdown of plant material. This
species is known as a wood rot fungus,
but it apparently attacks only decaying
plant material, not live plants.
iii. Effects on other organisms.
Peptaibols are toxic to Gram-positive
bacteria and various fungi. The
inhibitory action of peptaibols on
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various fungi is the reason that many
species of Trichoderma are used as
biocontrol agents of plant pathogenic
fungi. The peptaibol produced by T.
reesei, QM6a paracelsin, has been
shown to be inhibitory to one particular
fungus, Phoma destructiva.
Some species of Trichoderma,
specifically T. aggressivum, T.
pleuotrophilum, and T. fulvidum are
pathogens of mushrooms. However, T.
reesei QM6a is not a pathogen of
mushrooms.
6. Studies which indicate the survival
characteristics of the microorganism in
the environment. The species T. reesei
is known only from the single original
isolate QM6a from the Solomon Islands.
Therefore, there is little information on
its prevalence or behavior in the
environment. Microcosm studies have
been conducted that suggest it would
survive in the environment in the plant
rhizosphere and in bulk soils if
inadvertently released.
Although T. reesei was originally
isolated from a tropical climatic region,
it would be expected to persist in soils
for extended periods of time, even after
cold temperatures.
B. Evaluation of Available Information
Relevant to the Criteria for B.
amyloliquefaciens as a Recipient
Microorganism
1. Identification and classification of
the microorganism using available
genotypic and phenotypic information.
B. amyloliquefaciens was initially
proposed as a unique species in 1943.
The name B. amyloliquefaciens lost
standing when it was not included on
the Approved List of Bacterial Names
with Standing in Nomenclature in 1980.
Since classical phenotypic tests could
not differentiate it as a unique species
from Bacillus subtilis, it was regarded as
a subspecies of B. subtilis for several
decades. However, molecular evidence
from subsequent studies led to the
conclusion that B. amyloliquefaciens
did indeed deserve independent status.
The DNA homology between B. subtilis
and B. amyloliquefaciens is only about
15%. In addition, there were several
phenotypic properties that differed
between the two species.
Chemotaxonomic studies revealed
additional capability of separating
strains of B. amyloliquefaciens from the
other related species, Bacillus subtilis,
Bacillus licheniformis, and Bacillus
pumilus. The species has remained
within the genus Bacillus sensu stricto
since it was last established as a
separate species.
Recently, it has been proposed that
there are two subspecies within the
species B. amyloliquefaciens, B.
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amyloliquefaciens subsp.
amyloliquefaciens and B.
amyloliquefaciens subsp. plantarum.
The former subspecies includes the type
strain and likely most, if not all, of the
industrial strains of B.
amyloliquefaciens used for enzyme
production. The latter subspecies
consists of plant-associated strains used
as biocontrol agents due to the
production of several antifungal
lipopeptide and antibacterial polyketide
toxins. This exemption is restricted to
the subspecies B. amyloliquefaciens
subsp. amyloliquefaciens which
contains the industrial strains used for
enzyme production. Adequate genotypic
and phenotypic information is available
to accurately identify B.
amyloliquefaciens subsp.
amyloliquefaciens.
2. Information to evaluate the
relationship of the microorganism to
any other closely related
microorganisms which have a potential
for adverse effects on health or the
environment.
There are several species in the genus
Bacillus that are known pathogens.
These include Bacillus anthracis, which
is pathogenic to humans and other
animals, and Bacillus cereus, which is a
common cause of food poisoning.
Bacillus thuringiensis, Bacillus larvae,
Bacillus lentimorbus, Bacillus popilliae,
and some strains of Bacillus sphaericus
are pathogenic or toxigenic to certain
insects. The new subspecies Bacillus
amyloliquefaciens subsp. plantarum has
been shown to exhibit toxicity mainly to
plant pathogenic fungi but can also be
cytotoxic to mammalian cells. It is
possible, using polyphasic approaches,
to differentiate between B.
amyloliquefaciens subsp.
amyloliquefaciens and these other
species and subspecies that have the
potential to adversely affect humans or
other organisms. B. amyloliquefaciens
can be distinguished from the very
similar Bacillus subtilis by a few
phenotypic traits and DNA
dissimilarity.
3. A history of safe commercial use for
the microorganism.
B. amyloliquefaciens subsp.
amyloliquefaciens has been used to
produce commercial enzymes for more
than 50 years. It produces
carbohydrases, proteases, nucleases,
xylanases, and phosphatases that have
applications in the food, brewing,
distilling, and textile industries.
For commercial enzyme production,
B. amyloliquefaciens subsp.
amyloliquefaciens is grown in a closed
submerged fermentation. In submerged
fermentation, growth of the
microorganism occurs beneath the
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surface of the liquid growth medium.
The fermentation broth is a defined
mixture of carbon and nitrogen sources,
minerals, salts, and other nutrients that
is maintained at optimal pH and
temperature. These conditions support
the active growth and productivity of
the organisms. Submerged fermentation
systems reduce the potential for
exposure of workers to the production
organism and fermentation broth
aerosols, reduce the potential for
contamination of the culture, and make
the collection of extracellular enzyme
simpler and less costly. The
fermentation process is terminated
before the B. amyloliquefaciens subsp.
amyloliquefaciens organisms enter the
stationary growth phase, and the
production organisms are separated
from the fermentation broth and
inactivated. The enzyme preparation
may also be subjected to other
purification processes.
B. amyloliquefaciens subsp.
amyloliquefaciens has a long history of
safe use for enzyme production in food
and industrial applications with no
incidences associated with human
pathogenicity. In response to a petition
from the ETA, FDA affirmed that
carbohydrase enzyme preparations and
protease enzyme preparations derived
from either Bacillus subtilis or Bacillus
amyloliquefaciens are GRAS for use as
direct food ingredients. The European
Food Safety Authority (EFSA) has put B.
amyloliquefaciens on their list of
bacteria that have a ‘‘qualified
presumption of safety’’ because of a long
history of apparent safe use in food and
feed production. However, it was put on
the list with a qualifier that only strains
of B. amyloliquefaciens that do not have
toxigenic potential be used.
One strain of B. amyloliquefaciens has
been used as a biopesticide. A naturally
occurring strain of B. amyloliquefaciens
subsp. plantarum was registered in 2000
as a biopesticide active ingredient under
the Federal Insecticide, Fungicide, and
Rodenticide Act. It can only be used on
certain ornamental, non-food plants in
greenhouses and other closed structures.
4. Commercial uses indicating that
the microorganism products might be
subject to TSCA.
It is expected that intergeneric strains
of B. amyloliquefaciens subsp.
amyloliquefaciens would be used to
produce enzymes and to manufacture
other industrial chemicals subject to
TSCA. Many enzymes produced by B.
amyloliquefaciens, particularly aamylase, are used in laundry detergents
and in textile processing. B.
amyloliquefaciens also makes a
surfactant known as surfactin which
functions as an antibiotic.
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5. Studies which indicate the
potential for the microorganism to cause
adverse effects to health or the
environment.
a. Human health hazards— i.
Pathogenicity. B. amyloliquefaciens is
not pathogenic to humans. There are no
reports in the literature associating B.
amyloliquefaciens with infection or
disease in humans. B. amyloliquefaciens
has been categorized as a Biosafety
Level 1(BSL1) microorganism by the
Centers for Disease Control and
Prevention (CDC). BSL1 microorganisms
are well-characterized agents not known
to consistently cause disease in
immunocompetent adult humans, and
which present minimal potential hazard
to laboratory personnel and the
environment. Animal toxicity studies
were performed with B.
amyloliquefaciens strain FZB24 to
support its registration as a biopesticide.
Tests for acute oral toxicity/
pathogenicity, acute pulmonary
toxicity/pathogenicity, and acute
injection toxicity/pathogenicity showed
little to no adverse effects, which
indicated low mammalian toxicity and
a lack of pathogenicity/infectivity.
ii. Toxins and other secondary
metabolites. Although another species
in the genus Bacillus, B. cereus, has the
potential to produce food poisoning
toxins which cause both emetic and
diarrheal syndromes, and a variety of
local and systemic infections, the risk of
food-borne disease caused by bacilli
other than B. cereus is generally
considered to be negligible because
usually only B. cereus has the genes that
encode food poisoning toxins. Industrial
strains of Bacillus species belonging to
the Bacillus subtilis group, which
includes B. amyloliquefaciens, do not
express B. cereus toxins. In addition,
there are no reported cases of food
poisoning associated with B.
amyloliquefaciens.
Some strains of B. amyloliquefaciens
have been shown to produce bioactive
cyclic lipopeptide metabolites such as
iturin, surfactin, fengycin, and
bacillomycin D. These are cyclical
lipoprotein biosurfactants produced by
non-ribosomal peptide synthesis. They
have a low mammalian toxicity as
demonstrated by a lethal dose of 50%
(LD50) of >2,500 milligram/kilogram
(mg/kg) in an acute toxicity test of
surfactin C, and a no observed adverse
effect level of 500 mg/kg-day in a repeat
dose oral gavage study. Some strains of
B. amyloliquefaciens may also produce
the polyketide toxins macrolactin,
bacillanene, and difficidin. B.
amyloliquefaciens also produces the
protein toxin barnase and the antifungal
protein baciamin.
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There are reports of the isolation of B.
amyloliquefaciens from water-damaged
buildings in which occupants were
suffering ill health symptoms. Extracts
from biomass of isolated strains of
Bacillus exhibiting antifungal properties
were assessed for toxicity endpoints. All
of the isolated B. cereus and B.
amyloliquefaciens strains studied
showed cytotoxicity as evidenced by
inhibition of boar spermatozoa motility;
however, the B. amyloliquefaciens
strains affected boar spermatozoa
differently from the indoor B. cereus
isolates and the reference foodpoisoning strain.
The isolation of cytotoxic strains of B.
amyloliquefaciens from water-damaged
buildings is of little concern in relation
to the exemption of B.
amyloliquefaciens subsp.
amyloliquefaciens. It is important to
note that the Bacillus amyloliquefaciens
strains studied in water-damaged
buildings were specifically selected for
further study because the isolates
exhibited antifungal activity. Some of
the secondary metabolites produced by
these strains of B. amyloliquefaciens
also exhibited cytotoxicity to
mammalian cells (i.e., boar
spermatozoa). However, industrial
strains of B. amyloliquefaciens that are
classified as B. amyloliquefaciens subsp.
amyloliquefaciens have been shown not
to produce most, if not all, of the
antifungal and antibacterial
lipopeptides and polyketides produced
by the biocontrol-type strains. The
genome of the type strain of B.
amyloliquefaciens DSM 7T (now B.
amyloliquefaciens subsp.
amyloliquefaciens) is very similar to the
genome of the biocontrol strain FZB42
(B. amyloliquefaciens subsp.
plantarum). However, the latter
subspecies had genomic islands
carrying prophage sequences,
transposases, integrases, and
recombinases that the DSM 7T type
strain did not have. The DSM 7T type
strain was shown to have a diminished
capacity to non-ribosomally synthesize
secondary metabolites with antifungal
and antibacterial activities. The DSM 7T
type strain could not produce the
polyketides difficidin or macrolantin,
and could not produce lipopeptide such
as iturin, macrolantin, and other
compounds except for the compound
surfactin.
Although there are isolated reports of
toxin production in several antifungal,
environmental isolates of B.
amyloliquefaciens, the larger body of
studies available on the safety and
toxicity of B. amyloliquefaciens strains
used industrially for enzyme production
(Ref. 6) indicate that these strains are
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safe and non-toxic. For example, the
industrial strains of B.
amyloliquefaciens, Bacillus subtilis, and
Bacillus licheniformis used for largescale enzyme production did not exhibit
any cytotoxicity in Chinese hamster
ovary tests. In Europe, the toxicity of
two strains of B. amyloliquefaciens used
in the production of a-amylase and
bacillolysin was assessed by EFSA’s
Scientific Panel on Additives and
Products or Substances used in Animal
Feed. The panel concluded that the B.
amyloliquefaciens production strains
DSM9553 and DSM9554, when used as
a source of extracellular enzyme, do not
present a toxigenic risk. Given its
widespread distribution in the
environment, its long history of safe use
in industrial fermentation, the absence
of reports on pathogenicity to humans,
and the limited reports of cytotoxicity,
EPA concludes that the use of B.
amyloliquefaciens in fermentation
facilities for production of enzymes or
specialty chemicals does not present a
human health concern.
b. Environmental hazards— i.
Hazards to animals. There are no
reports suggesting that B.
amyloliquefaciens is pathogenic to
domesticated animals or wildlife. The
cytotoxicity of antifungal secondary
metabolites to mammalian cells by
biocontrol strains of B.
amyloliquefaciens subsp. plantarum is
discussed in this Unit.
ii. Hazards to plants. B.
amyloliquefaciens is not pathogenic to
plants. The plant-associated strains of B.
amyloliquefaciens are beneficial to
plants because they inhibit the growth
of fungal plant pathogens. Antifungal
and antibacterial secondary metabolites
produced by strains of B.
amyloliquefaciens such as iturins,
surfactins, fengycin, bacillomycins, and
azalomycin have been shown to inhibit
the growth of Rhizoctonia solani,
Xanthomonas campestris pv.
campestris, Alternaria brassicae, Botyris
cinerea, Leptosphaeria maculans,
Verticillium longisporum, Pythium
ultimatum, Aspergillus spp., Fusarium
spp., Bipolaris sorokiniana, and
Fusarium oxysporum.
In addition to producing antifungal
and antibacterial compounds, B.
amyloliquefaciens is known as a plant
growth-promoting rhizobacterium, and
some of the biological control strains of
B. amyloliquefaciens were shown to
produce the phytohormone indole-3acetic acid.
6. Studies which indicate the survival
characteristics of the microorganism in
the environment.
Several studies assessing the survival
of B. amyloliquefaciens are available in
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the public literature and are described
in EPA’s Risk Assessment of B.
amyloliquefaciens (Ref. 6). Given that
the natural habitat for B.
amyloliquefaciens is typically in soil, on
plant roots, or as an endophyte within
the roots or stems of plants, the
bacterium is likely to survive for a least
some period of time if inadvertently
released to the environment. However,
like other bacilli, survival in soil may
occur predominately as the resistant
endospore state, whereas in the
rhizosphere, it may exist as active
vegetative cells.
VI. Physical Containment and Control
Technologies for T. reesei QM6a and
B. amyloliquefaciens subsp.
amyloliquefaciens
A. Release and Exposure Assessment in
Support of the TSCA Section 5(h)(4)
Exemption for T. reesei QM6a
The estimated releases of the
microorganism from an enzyme
manufacturing facility and exposures of
workers, the general population, and the
environment to the microorganisms are
based on a generic scenario developed
by EPA in 1997 for large-scale closed
system enzyme fermentation. The
generic scenario assumes the facility
operates 350 days/year, produces 100
batches/year, the maximal cell
concentration in the fermentation broth
is 1 x 107 colony-forming units (cfu)/ml,
and the volume of the fermentation
broth is 70,000 L. The process consists
of the main steps of laboratory
propagation, fermentation, inactivation,
and recovery where filtration operations
separate out the microbial biomass from
the concentrated desired product. The
operations, sources of exposure and
release are described in more detail in
EPA’s Release and Exposure Assessment
(Ref. 13).
Exposures of workers to the
microorganisms in during processing
operations using submerged standard
industrial fermentation do not pose
concerns. The release of microbial cells
in aerosols or in liquid and solid waste
streams in submerged standard
industrial fermentation operations with
the containment and inactivation
conditions of the Tier I exemption, are
considered low. Thus, potential
exposures to the general human
population to the microorganism
through inhalation or drinking water
ingestion and to the environment are
also low.
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B. Release and Exposure Assessment in
Support of the TSCA Section 5(h)(4)
Exemption for B. amyloliquefaciens
subsp. amyloliquefaciens
subpart G, relating to the introduced
genetic material, and the physical
containment of the new
microorganisms, have been met.
The estimated releases of the
microorganism from an enzyme
manufacturing facility and exposures of
the microorganisms to workers, the
general population, and the
environment are based on a generic
scenario developed by EPA in 1997 for
large-scale closed system enzyme
fermentation. The generic scenario
assumes the facility operates 350 days/
year, produces 100 batches/year, the
maximal cell concentration in the
fermentation broth is 1 × 1011 cfu/ml
and the volume of the fermentation
broth is 70,000 L. The process consists
of the main steps of laboratory
propagation, fermentation and then
recovery where filtration operations
separate out the biomass from the
concentrated desired product. The
operations, sources of exposure and
release are described in more detail in
EPA’s Release and Exposure Assessment
(Ref. 14).
Exposures of workers to the
microorganisms during processing
operations using submerged standard
industrial fermentation do not pose
concerns. The release of microbial cells
in aerosols or in liquid and solid waste
streams in submerged standard
industrial fermentaion operations with
the containment and inactivation
conditions of the Tier I exemption are
considered low. Thus, potential
exposures to the general human
population to the microorganism
through inhalation or drinking water
ingestion and to the environment are
also low.
A. Risk Assessment for T. reesei QM6a
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VII. Risk Assessment Overview for T.
reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens
EPA’s Risk Assessment documents
(Refs. 5 and 6) provide more detailed
information, and supporting references,
for EPA’s evaluation of the available
information and the potential risks to
health and the environment. EPA has
determined that because of the low
hazard potential and safe history of use
of T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens, the TSCA section
5(h)(4) exemption will not present an
unreasonable risk of injury to health or
the environment, including an
unreasonable risk of injury to a
potentially exposed or susceptible
subpopulation under the conditions of
use, provided that the other conditions
of the exemptions at 40 CFR part 725,
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There is only one potential concern
for human health and environmental
hazards associated with T. reesei QM6a,
and that is for paracelsin production.
Paracelsin production is not expected to
occur in submerged standard industrial
fermentation operations conducted
solely for growth of the microorganism
to produce enzymes. There is no
concern for potential pathogenicity of T.
reesei QM6a to humans, plants,
domesticated animals, or wildlife. The
body of evidence of pathogenicity
testing on various industrial strains
indicates that T. reesei is not pathogenic
to humans. Toxicity testing on a number
of enzymes produced by T. reesei
indicates that the fungus does not
produce toxins when used in the
submerged standard industrial
fermentation operations used for
enzyme production.
T. reesei has a long history of safe use
and is expected to present low hazard
to workers, the general public, and the
environment. Although direct
monitoring data are unavailable,
estimates of potential exposures made
by EPA in its assessment of potential
risks (Ref. 5) do not indicate high levels
of exposure of T. reesei to either
workers or the public from submerged
standard industrial fermentation
operations used for enzyme production.
Standard industrial hygiene
management practices currently used in
the fermentation industry reduce the
potential for adverse health effects in
the workplace. The use of engineering
controls (closed fermentation systems),
appropriate work practices, personal
protective equipment, and personal
hygiene reduce the potential for worker
exposure. Thus, current practices
reduce the potential for the dermal and
respiratory exposures estimated by EPA.
Based on worst-case exposure
scenarios and toxicity of the
microorganism, EPA has made the
determination that the potential risk to
workers, the general public, and to the
environment resulting from the use of T.
reesei QM6a in submerged standard
industrial fermentation operations used
for enzyme production is low, provided
the additional criteria of the tiered
exemptions for the introduced genetic
material and the physical containment
conditions are met (Ref. 5).
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B. Risk Assessment for B.
amyloliquefaciens subsp.
amyloliquefaciens
Industrial strains of B.
amyloliquefaciens subsp.
amyloliquefaciens are not pathogenic to
humans, plants, domesticated animals,
or wildlife, and do not produce many of
the toxic secondary metabolites found
in biological control strains of B.
amyloliquefaciens subsp. plantarum.
The long history of safe use of enzymes
produced by industrial strains of B.
amyloliquefaciens in food is evidence
that the bacterium does not produce
toxins under standard conditions used
for enzyme production.
Current practices in the fermentation
industry reduce the potential for
adverse health effects in the workplace.
The use of engineering controls (closed
fermentation systems), appropriate work
practices, personal protective
equipment, and personal hygiene
reduce the potential for worker
exposure and reduce the potential for
the dermal and respiratory exposures.
Industrial strains of B.
amyloliquefaciens have a long history of
safe use and are expected to present low
hazard to workers, the general public,
and the environment. Although direct
monitoring data are unavailable,
exposure estimates do not suggest high
levels of exposure of B.
amyloliquefaciens subsp.
amyloliquefaciens to either workers or
the public resulting from the industrial
fermentation procedures that are
standard throughout the industry.
Based on worst-case exposure
scenarios and toxicity of the
microorganism, EPA has made the
determination that the potential risk to
workers, the general public, and the
environment associated with the use of
industrial strains of B.
amyloliquefaciens subsp.
amyloliquefaciens in submerged
standard industrial fermentation is low
provided the additional criteria of the
tiered exemptions for the introduced
genetic material and the physical
containment conditions are met (Ref. 6).
VIII. Rationale for Adding T. reesei
QM6a and B. amyloliquefaciens
subsp. amyloliquefaciens to the List of
Recipient Microorganisms at 40 CFR
725.420
A. Statutory Background
On June 22, 2016, the ‘‘Frank R.
Lautenberg Chemical Safety for the 21st
Century Act,’’ amended TSCA (15
U.S.C. 2601 et seq.) (Ref. 15). Pursuant
to TSCA section 5(h)(4), EPA is
authorized, upon request and by rule, to
exempt the manufacturer of any new
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chemical substance from all or part of
the requirements of TSCA section 5 if
EPA determines that the manufacture,
processing, distribution in commerce,
use, or disposal of the chemical
substance, or any combination of such
activities, will not present an
unreasonable risk of injury to human
health or the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation
identified by the Administrator under
the conditions of use. The amended
language of the statute with regard to
section 5(h)(4) did not alter EPA’s
approach to balancing the
considerations of the costs and benefits
of issuing an exemption rule.
B. EPA’s Approach for Assessing
‘‘Unreasonable Risk’’ for T. reesei QM6a
and B. amyloliquefaciens subsp.
amyloliquefaciens
In determining whether T. reesei
QM6a and B. amyloliquefaciens subsp.
amyloliquefaciens will not present an
unreasonable risk of injury to human
health or the environment, the Agency
considered more than just the inherent
risks presented by the two
microorganisms. The Agency also
considered the full range of societal
benefits associated with the exemption;
for example, as discussed in more detail
below, EPA considered not only the cost
savings to the users of the
microorganism, but also the societal
benefits that flow from promotion of the
use of low-risk recipient
microorganisms, while allowing the
Agency to direct its resources toward
reviewing higher risk microorganisms.
It is important that EPA is revising
one aspect of the existing tiered
exemptions at 40 CFR 725.420 by
expanding the exemption to apply to
two specific microorganisms. The
narrow scope of this action affected the
scope of EPA’s cost-benefit analysis in
which EPA compared the risks and
benefits of the two microorganisms
being considered for an exemption with
the risks that would have resulted if
those same two microorganisms
remained subject to full MCAN
submission requirements and 90-day
EPA review. EPA did not compare the
risks and benefits that would result from
use of these two microorganisms in the
absence of any regulation.
It is also significant that the standard
applicable to this rule is that the
microorganisms ‘‘will not present
unreasonable risk,’’ rather than ‘‘no
risk.’’ It is not possible to eliminate all
risks associated with the manufacture,
processing, distribution in commerce,
use, and disposal of any new
microorganism.
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C. Application of No Unreasonable Risk
Factors for T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens
The following is an explanation of the
factors and their analyses relevant to the
no unreasonable risk finding.
1. Risks associated with these two
microorganisms. EPA’s evaluation of the
available information concerning T.
reesei QM6a and B. amyloliquefaciens
subsp. amyloliquefaciens against these
criteria is presented in detail in Unit V.,
and is summarized again here for the
readers’ convenience.
The Agency developed specific
criteria in 40 CFR 725.67 that the
Agency uses in determining the extent
of a potential recipient microorganism’s
risks, and its eligibility for listing at 40
CFR 725.420. These criteria were
explained in detail in the proposed
‘‘biotech’’ rule (Ref. 16), the final
‘‘biotech’’ rule (Ref. 17), and are
discussed in Unit V. EPA’s conclusions
for these two microorganisms are based
on the available data and EPA’s
experience under 40 CFR part 725. T.
reesei QM6a is not pathogenic to
humans, plants, domesticated animals,
or wildlife and the fungus does not
produce toxins under submerged
standard industrial fermentation
operations used for enzyme production.
T. reesei QM6a has a long history of safe
use and is generally expected to present
low risk to workers, the general public,
and the environment resulting from
submerged standard industrial
fermentation operations used for
enzyme production that are standard
throughout the industry.
Under non-standard conditions of
fermentation, such as with the
deliberate fermentation of cellulosic
biomass for saccharification of plant
material or extended fermentation,
paracelsin may be produced. The risks
associated with the production of
paracelsin may be significant due to its
toxicity to mammalian cells, aquatic
species, Gram-positive bacteria, and
various fungi. However, the potential
risk associated with paracelsin
production is expected to be
significantly reduced by this rule, which
limits the exemption to fermentation
operations using submerged standard
industrial fermentation operations used
for enzyme production.
Industrial strains of B.
amyloliquefaciens subspecies
amyloliquefaciens are not pathogenic to
humans, plants, domesticated animals,
or wildlife, and do not produce toxins
under standard conditions used for
enzyme production. Industrial strains of
B. amyloliquefaciens subsp.
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amyloliquefaciens used for the
production of enzymes have a long
history of safe use and are expected to
present low hazards to human health
and the environment.
Only strains of B. amyloliquefaciens
that fall into the subspecies B.
amyloliquefaciens amyloliquefaciens
were considered as the eligible recipient
microorganism at 40 CFR 725.420. In
this rule, EPA is excluding other strains/
subspecies of these two species for
which:
• The Agency has insufficient data
and review experience to find that they
will not present an unreasonable risk of
injury or
• The Agency has found that, under
certain conditions, based on data on the
species in question, a strain or
subspecies may present an unreasonable
risk, thereby requiring a closer
examination of the conditions of
manufacturing, processing, distribution
in commerce, use, and disposal during
a 90-day MCAN review. Consequently,
additional information would be
necessary to make an appropriate
determination about the organisms’
potential risks.
The Agency believes that the
requirement for submission of a MCAN
followed by a 90-day review period for
new intergeneric microorganisms that
use T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens as recipient
microorganisms is not necessary to
address the risks associated with these
microorganisms and would not result in
any additional protection than would be
achieved by this rule. This conclusion is
based, in part, on EPA’s findings
regarding the intrinsically low level of
hazard that these two organisms pose to
human health and the environment. The
requirements of the Tier I and Tier II
exemptions and the restrictions in this
rule on fermentation conditions place
sufficient constraints to significantly
limit the potential risks of injury to
human health or the environment,
including potential risks to potentially
exposed or susceptible subpopulations
under the conditions of use. In making
this determination, EPA identified
workers as a potentially exposed or
susceptible subpopulation to the
substance under the conditions of use
and concluded that, with the limitations
described above, the substances will not
present an unreasonable risk of injury to
health or the environment.
The Agency concludes that the
criteria set forth in this rule are
sufficient to mitigate the identified risks
associated with these microorganisms.
Because of the low hazard potential and
safe history of use of T. reesei QM6a and
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B. amyloliquefaciens subsp.
amyloliquefaciens, EPA concludes that
the TSCA section 5(h)(4) exemption will
not present an unreasonable risk of
injury to health or the environment,
including an unreasonable risk of injury
to a potentially exposed or susceptible
subpopulation under the conditions of
use, provided that the other conditions
of the exemptions at 40 CFR part 725,
subpart G, relating to the introduced
genetic material, and the physical
containment of the new
microorganisms, have been met.
2. Costs. As discussed in Unit X., this
rule is anticipated to reduce costs to
currently regulated entities in the long
run. Expanding the list of recipient
microorganisms eligible for exemption
does not otherwise impose any
additional cost or other burden on
currently regulated entities, or existing
fermentation processes.
Limiting the use of this exemption to
the identified fermentation conditions is
also estimated to impose no burden on
affected entities. The restriction merely
codifies existing industrial fermentation
procedures for manufacturing
operations that currently seek to use
tiered exemptions. Consequently, EPA
expects that most, if not all,
manufacturers using these microbes
would already have the measures in
place to qualify for the exemption.
Equally important, this limitation would
add no burden to any existing
fermentation processes. Currently,
fermentation operations with either of
these microbes are not eligible for the
tiered exemption, and thus a MCAN
must be submitted. Any company that
chooses to use a different fermentation
process could continue to operate under
the status quo and simply submit a
MCAN. This rule simply offers an
additional, less costly option, to
facilities that choose to use the
fermentation operations discussed in
this rule.
3. Benefits. The following discussion
describes the benefits of expanding the
list of recipient microorganisms eligible
for exemption in a qualitative manner;
for a more quantitative approach, see
the economic analysis prepared for this
rule (Ref. 18). A summary of that
economic analysis is also provided in
Unit IX.
The benefits analyzed encompass
more than the direct benefits associated
with submitting a Tier I or Tier II
exemption for a new intergeneric
microorganism rather than a MCAN.
EPA’s benefit analysis included a
consideration of the broader benefits to
society. EPA’s unreasonable risk
determination is based on broader
benefits to society as well as those
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benefits attributable to a reduction in
the burden associated with submission
of Tier I and Tier II exemptions rather
than MCANs.
EPA has concluded that
manufacturers of new intergeneric
microorganisms based on these low-risk
microorganisms currently bear an
unnecessary regulatory burden. By
adding T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens to the list of eligible
recipient microorganisms in 40 CFR
725.420, the Agency removes
unnecessary regulatory impediments to
the design, manufacture, and
commercialization of these low risk new
intergeneric microorganisms, and of the
chemical substances that can be
produced by these safer
microorganisms. This action will also
reduce the costs associated with
industry’s reporting burden, including
the costs associated with the
preparation of the submission, and with
the delay in the commercial market
introduction of the new intergeneric
microorganism. Some of the costsavings benefits may accrue to small
businesses, either as developers of the
exempt microorganisms, as producers of
fermentation chemicals using the live
microorganisms, or as customers for
enzymes or other products made using
the microorganisms.
There will also be a reduction in the
Agency review resources currently
allocated to reviews of MCANs for these
two microorganisms. These Agency
resources will be shifted to the review
of new intergeneric microorganisms or
chemical substances of greater concern.
The addition of the two
microorganisms to the list of
microorganisms eligible for exemption
is expected to encourage innovation in
the industry. It is reasonable to assume
that a new intergeneric microorganism
would either possess a new function or
serve an existing function more
efficiently or at a lower cost. The
reduction in delay for that new
intergeneric microorganism to be
introduced into commerce is expected
to be a benefit to both manufacturers
and the general public who will have
access to the substance more quickly.
The expected benefits to innovation
have not been quantified but include:
Reduced time to develop and
commercialize organisms; decreased
cost of some downstream industrial
products, such as fuel ethanol;
improved consumer appeal of some
products, such as certain textiles; and
reduced costs of some consumer
products, such as detergent and leather
goods.
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4. Risk/benefit balance. Determining
the presence or absence of an
unreasonable risk for purposes of
issuing an exemption pursuant to TSCA
section 5(h)(4) requires balancing of the
benefits and risks posed by a regulatory
action. EPA has determined that the
risks are generally low based on the
inherent properties and intended uses of
T. reesei QM6a and B.
amyloliquefaciens subsp.
amyloliquefaciens and will be
adequately managed by the restrictions
in the rule, combined with the existing
requirements of the Tier I and Tier II
exemptions.
EPA anticipates that expanding the
list of microorganisms eligible for
exemption will impose no costs and
will reduce costs to currently regulated
entities that use those recipients. The
limitation to certain fermentation
conditions is not a cost that will be
imposed by this rule but rather a
limitation on the amount of regulatory
relief it will provide. The limitations on
fermentation conditions reflect
industrial fermentation procedures that
are currently common practices for the
affected industry.
EPA has also concluded that the
benefits of the addition of T. reesei
QM6a and B. amyloliquefaciens subsp.
amyloliquefaciens as recipient
microorganisms to the list of recipient
microorganisms at 40 CFR 725.420 are
quite significant. This addition reduces
the overall regulatory burden for
affected entities by reducing the
reporting requirements and by
eliminating the delay of these products
into commerce. The rule benefits both
regulated entities and the general public
by promoting the expedited
manufacture and use of the chemical
substances produced using these lowrisk organisms and manufacturing
processes. There is also the added
benefit of concentrating limited EPA
resources on regulation of chemical
substances which have a greater
potential to present significant risks,
rather than on these two
microorganisms. While this is difficult
to quantify, it is considered substantial.
In sum, the criteria set forth in this
exemption are sufficient to mitigate the
low level of potential risks presented by
these organisms, particularly when
compared to the benefits, in toto, of this
exemption, to levels that are consistent
with the statutory standard for an
exemption. Consequently, EPA has
determined that adding T. reesei QM6a
and B. amyloliquefaciens subsp.
amyloliquefaciens as recipient
microorganisms to the list of recipient
microorganisms at 40 CFR 725.420 is
appropriate. The two microorganisms
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will not present an unreasonable risk of
injury to human health or the
environment when manufactured under
the conditions of this exemption.
IX. Economic Impacts
EPA’s economic analysis (Ref. 18)
evaluates the potential for significant
economic impacts as a result of the
addition of two microorganisms (T.
reesei QM6a and B. amyloliquefaciens
subsp. amyloliquefaciens) to 40 CFR
725.420, which lists recipient
microorganisms eligible for Tier I and
Tier II exemptions. Over the course of
the first 10 years after the effective date
of the final rule, EPA estimates that the
addition of the two microorganisms to
the list will generate a total cost savings
to society of approximately $4.5 million.
Industry is estimated save
approximately $2.7 million and the
Agency approximately $1.8 million. The
equivalent, annualized cost savings to
industry are expected to be $260,000 per
year and $252,000 per year at a 3% and
7% discount rate, respectively. EPA
estimates that there will be a net
decrease in burden to industry of 27,864
hours over this 10-year period.
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X. Scientific Standards, Evidence, and
Available Information
EPA has used scientific information,
technical procedures, measures,
methods, protocols, methodologies, and
models consistent with the best
available science, as applicable. These
sources supply information relevant to a
determination that the microorganisms
subject to this rule will not present an
unreasonable risk of injury to health or
the environment, including an
unreasonable risk to a potentially
exposed or susceptible subpopulation
identified by the Administrator under
the conditions of use. The clarity and
completeness of the data, assumptions,
methods, quality assurance, and
analyses employed are documented, as
applicable and to the extent necessary
for purposes of this rule, in Units V.
through VIII. and in the references. The
extent to which the various information,
procedures, measures, methods,
protocols, methodologies or models
used in EPA’s decision have been
subject to independent verification or
peer review is adequate to justify their
use, collectively, in the record for this
rule.
XI. References
The following is a listing of the
documents that are specifically
referenced in this document. The docket
includes these documents and other
information considered by EPA,
including documents that are referenced
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within the documents that are in the
docket, even if the referenced document
is not physically located in the docket.
For assistance in locating these other
documents, please consult the technical
person listed under FOR FURTHER
INFORMATION CONTACT.
1. Genencor International, Inc. Letter of
Application to list Trichoderma reesei as
exempt under subpart G of 40 CFR part 725—
Reporting Requirements and Review
Processes for Microorganisms. March 17,
2005.
2. Novo Nordisk BioChem North America,
Inc. Letter of Application to list Bacillus
amyloliquefaciens as exempt under subpart G
of 40 CFR part 725—Reporting Requirements
and Review Processes for Microorganisms.
November 7, 1997.
3. EPA, OPPT. Email confirming Novo
Nordisk BioChem North America, Inc.’s letter
of application to list Bacillus
amyloliquefaciens as exempt under subpart G
of 40 CFR part 725—Reporting Requirements
and Review Processes for Microorganisms.
August 3, 2009.
4. US EPA. Microorganisms; General
Exemptions from Reporting Requirements;
Revisions to Recipient Organisms Eligible for
Tier I and Tier II Exemptions; Proposed Rule.
RIN 2070–AJ65; FRL–9348–1. 77 FR 54499,
September 5, 2012. (‘‘2012 Proposed Rule’’).
5. EPA, OPPT. Risk Assessment of
Trichoderma reesei for Consideration of
Addition to the List of Eligible Recipient
Microorganisms for the 5(h)(4) Exemptions
from MCAN Reporting Requirements.
October 2011.
6. EPA, OPPT. Risk Assessment of Bacillus
amyloliquefaciens subsp. amyloliquefaciens
for Consideration of Addition to the List of
Eligible Recipient Microorganisms for the
5(h)(4) Exemptions from MCAN Reporting
Requirements. July 2015.
7. Anonymous Public Comment, Document
ID: EPA–HQ–OPPT–2011–0740–0015;
October 23, 2012.
8. Richard Fitti, West Chester University of
PA Comment, Document ID: EPA–HQ–
OPPT–2011–0740–0017; November 5, 2012.
9. Anthony T. Pavel, General Counsel &
Secretary, Enzyme Technical Association
(ETA) and Rina Singh, Director of Policy,
Science & Renewable Chemicals, Industrial
and Environmental Section, Biotechnology
Industry Organization (BIO) Comment,
Document ID EPA–HQ–OPPT–2011–0740–
0016; November 2012.
10. ETA. Supplemental information on
Trichoderma reesei. January 29, 2010.
11. ETA. Supplemental information on
Trichoderma reesei. June 16, 2011.
12. Nevalainen, H., P. Suominen, K.
Tasimisto. 1994. On the safety of
Trichoderma reesei. J. Biotechol. 37:193–200.
13. EPA, OPPT. Release and Exposure
Assessment in Support of the TSCA Section
5(h)(4) Exemption for Trichoderma reesei.
June 2011.
14. EPA, OPPT. Release and Exposure
Assessment in Support of the TSCA Section
5(h)(4) Exemption for Bacillus
amyloliquefaciens. June 2011.
15. Legislative History of the Toxic
Substances Control Act, pp. 409–423. House
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13771
Report 1341, 94th Congress, 2nd Session.
1976.
16. EPA. Microbial Products of
Biotechnology; Proposed Regulation under
the Toxic Substances Control Act. Federal
Register (59 FR 45526; September 1, 1994)
(FRL–4774–4).
17. EPA. Microbial Products of
Biotechnology; Final Regulation under the
Toxic Substances Control Act. Federal
Register (62 FR 17910; April 11, 1997) (FRL–
5577–2).
18. EPA, OPPT. Economic Analysis for the
Final Biotechnology Exemptions Rule for
Trichoderma reesei and Bacillus
amyloliquefaciens. October 2019.
XII. Statutory and Executive Order
Reviews
Additional information about these
statutes and Executive Orders can be
found at https://www2.epa.gov/lawsregulations/laws-and-executive-orders.
A. Executive Order 12866: Regulatory
Planning and Review and Executive
Order 13563: Improving Regulations
and Regulatory Review
This action is not a significant
regulatory action and was therefore not
submitted to the Office of Management
and Budget (OMB) for review under
Executive Orders 12866 (58 FR 51735,
October 4, 1993) and 13563 (76 FR 3821,
January 21, 2011).
B. Executive Order 13771: Reducing
Regulations and Controlling Regulatory
Costs
This is considered a deregulatory
action under Executive Order 13771 (82
FR 9339, February 3, 2017) because this
rule is expected to provide meaningful
burden reduction by adding T. reesei
and B. amyloliquefaciens subspecies
amyloliquefaciens to the list of recipient
microorganisms that may be used to
qualify for the Tier I and Tier II
exemptions from full notification and
reporting under TSCA for new
microorganisms that are being
manufactured for introduction into
commerce. The rule is expected to
generate cost savings for organizations
that, in the absence of the rule, would
submit MCANs for new intergeneric T.
reesei or B. amyloliquefaciens strains.
EPA estimates that the rule will result
in cost savings for both industry and the
Agency.
C. Paperwork Reduction Act (PRA)
This action does not impose any new
information collection requirements or
related burden that would require
additional review or approval by OMB
under the PRA, 44 U.S.C. 3501 et seq.
The information collection activities
associated with the submission of Tier
1 and Tier 2 notices under TSCA have
already been approved by OMB
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pursuant to the PRA and are covered by
the following existing Information
Collection Requests (ICRs): OMB control
numbers 2070–0012 (EPA ICR No.
0574.15) and 2070–0038 (EPA ICR No.
1188.11). In granting these exemptions,
this rule does not impose any new
information collection requirements and
is expected to reduce the amount of
required reporting by allowing firms to
submit less information for qualifying
microorganisms. Over the ten-year
period, industry is expected to subtract
a total of 27,864 hours at an average of
2,786 hours per year.
D. Regulatory Flexibility Act (RFA)
Pursuant to section 605(b) of the RFA,
5 U.S.C. 601 et seq., I certify that this
final rule will not have a significant
economic impact on a substantial
number of small entities. In making this
determination, EPA believes that the
impact of concern is any adverse
economic impact on small entities, and
that EPA may certify that a rule will not
have a significant economic impact on
a substantial number of small entities if
the rule relieves regulatory burden, has
no net burden or otherwise has a
positive economic effect on the small
entities subject to the rule. This action
establishes exemptions from existing
requirements that apply regardless of
the size of the entity. The factual basis
for this certification is presented in the
small entity impact analysis that was
prepared as part of the Economic
Analysis for this rule (Ref. 18) and is
briefly summarized in Unit VIII.
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E. Unfunded Mandates Reform Act
(UMRA)
This action does not contain an
unfunded mandate as described in
UMRA, 2 U.S.C. 1531–1538, and does
not significantly or uniquely affect small
governments. This action is not
expected to impose enforceable duty on
any state, local or tribal governments,
and the requirements imposed on the
private sector are not expected to result
in annual expenditures of $100 million
or more for the private sector. As such,
EPA has determined that the
requirements of UMRA sections 202,
203, 204, or 205 do not apply to this
action.
F. Executive Order 13132: Federalism
This action does not have federalism
implications as specified in Executive
Order 13132 (64 FR 43255, August 10,
1999). It will not have substantial direct
effects on the states, on the relationship
between the national government and
the states, or on the distribution of
power and responsibilities among the
various levels of government. EPA has
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16:53 Mar 09, 2020
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no information to indicate that any state
or local government commercially
manufactures or processes the
microorganisms covered by this action.
Thus, Executive Order 13132 does not
apply to this action.
G. Executive Order 13175: Consultation
and Coordination With Indian Tribal
Governments
This action does not have tribal
implications as specified in Executive
Order 13175 (65 FR 67249, November 9,
2000). It will not have substantial direct
effects on tribal governments, on the
relationship between the Federal
government and the Indian tribes, or on
the distribution of power and
responsibilities between the Federal
government and Indian tribes. EPA has
no information to indicate that any
tribal government commercially
manufactures or processes the
microorganisms covered by this action.
Thus, E.O. 13175 does not apply to this
action.
H. Executive Order 13045: Protection of
Children From Environmental Health
Risks and Safety Risks
EPA interprets Executive Order 13045
(62 FR 19885, April 23, 1997), as
applying only to those regulatory
actions that concern health or safety
risks, such that the analysis required
under section 5–501 of Executive Order
13045 has the potential to influence the
regulation. This action is not subject to
Executive Order 13045 because it does
not establish an environmental standard
intended to mitigate health or safety
risks.
I. Executive Order 13211: Actions That
Significantly Affect Energy Supply,
Distribution, or Use
This action is not a ‘‘significant
energy action’’ as defined in Executive
Order 13211 (66 FR 28355, May 22,
2001), because it is not a significant
regulatory action under Executive Order
12866, and is not likely to have a
significant adverse effect on energy
supply, distribution, or use.
J. National Technology Transfer and
Advancement Act (NTTAA)
Since this action does not involve any
technical standards, NTTAA section
12(d), 15 U.S.C. 272 note, does not
apply to this action.
K. Executive Order 12898: Federal
Actions to Address Environmental
Justice in Minority Populations and
Low-income Populations
This action does not entail special
considerations of environmental justice
related issues as delineated by
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Fmt 4700
Sfmt 4700
Executive Order 12898 (59 FR 7629,
February 16, 1994), because it does not
establish an environmental health or
safety standard.
VII. Congressional Review Act (CRA)
This action is subject to the CRA, 5
U.S.C. 801 et seq., and EPA will submit
a rule report to each House of the
Congress and to the Comptroller General
of the United States. This action is not
a ‘‘major rule’’ as defined by 5 U.S.C.
804(2).
List of Subjects in 40 CFR Part 725
Environmental protection,
Administrative practice and procedure,
Biotechnology, Chemicals, Hazardous
substances, Imports, Labeling,
Microorganisms, Occupational safety
and health, Reporting and
recordkeeping requirements.
Dated: March 4, 2020.
Alexandra Dapolito Dunn,
Assistant Administrator, Office of Chemical
Safety and Pollution Prevention.
Therefore, 40 CFR chapter I is
amended as follows:
PART 725—[AMENDED]
1. The authority citation for part 725
continues to read as follows:
■
Authority: 15 U.S.C. 2604, 2607, 2613, and
2625.
2. In § 725.3, add in alphabetical order
a definition for ‘‘Submerged standard
industrial fermentation’’ to read as
follows:
■
§ 725.3
Definitions.
*
*
*
*
*
Submerged standard industrial
fermentation means a fermentation
system that meets all of the following
conditions:
(1) Enzyme production is conducted
under conditions of submerged
fermentation (i.e., growth of the
microorganism occurs beneath the
surface of the liquid growth medium).
(2) Any fermentation of solid plant
material or insoluble substrates, to
which T. reesei fermentation broth is
added after the submerged standard
industrial fermentation operations used
for enzyme production is completed,
may be initiated only after the
inactivation of the microorganism as
delineated in 40 CFR 725.422(d).
*
*
*
*
*
■ 3. In § 725.420, add paragraphs (k)
and (l) to read as follows:
§ 725.420
Recipient microorganisms.
*
*
*
*
*
(k) Trichoderma reesei strain QM6a
and its derivatives used only in
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submerged standard industrial
fermentation operations as defined at 40
CFR 725.3.
(l) Bacillus amyloliquefaciens subsp.
amyloliquefaciens.
[FR Doc. 2020–04746 Filed 3–9–20; 8:45 am]
BILLING CODE 6560–50–P
FEDERAL COMMUNICATIONS
COMMISSION
47 CFR Part 54
[WC Docket Nos.19–126, 10–90; FCC 20–
5; FRS 16498]
Rural Digital Opportunity Fund,
Connect America Fund
Federal Communications
Commission.
ACTION: Final rule.
AGENCY:
In this document, the Federal
Communications Commission
(Commission) adopts the framework for
the Rural Digital Opportunity Fund. The
Rural Digital Opportunity Fund builds
on the Connect America Fund (CAF)
Phase II auction, which allocated funds
to deploy networks serving more than
700,000 unserved rural homes and
businesses across 45 states. The Rural
Digital Opportunity Fund represents the
Commission’s single biggest step to
close the digital divide and connect
millions more rural homes and small
businesses to high-speed broadband
networks.
SUMMARY:
Effective April 9, 2020, except of
§§ 54.313(e), 54.316(a)(8), (b)(5), (c)(1),
54.804 (a) through (c), and 54.806. The
Commission will publish a document in
the Federal Register announcing the
effective date of those rules.
FOR FURTHER INFORMATION CONTACT:
Alexander Minard, Wireline
Competition Bureau, (202) 418–7400 or
TTY: (202) 418–0484.
SUPPLEMENTARY INFORMATION: This is a
summary of the Commission’s Report
and Order (Order) in WC Docket Nos.
19–126, 10–90; FCC 20–5, adopted on
January 30, 2020 and released on
February 7, 2020. The full text of this
document is available for public
inspection during regular business
hours in the FCC Reference Center,
Room CY–A257, 445 12th Street SW,
Washington, DC 20554 or at the
following internet address: https://
www.fcc.gov/document/fcc-launches20-billion-rural-digital-opportunityfund-0.
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DATES:
I. Introduction
1. Bringing digital opportunity to
Americans living on the wrong side of
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16:53 Mar 09, 2020
Jkt 250001
the digital divide continues to be the
Federal Communication Commission’s
top priority. It is imperative that the
Commission take prompt and
expeditious action to deliver on its goal
of connecting all Americans, no matter
where they live and work. Without
access to broadband, rural communities
cannot connect to the digital economy
and the opportunities for better
education, employment, healthcare, and
civic and social engagement it provides.
2. In recent years, the Commission has
made tremendous strides toward its goal
of making broadband available to all
Americans. But while the digital divide
is closing, more work remains to be
done. Therefore, in the Order, the
Commission adopts the framework for
the Rural Digital Opportunity Fund. It
builds on the successful model from
2018’s CAF Phase II auction, which
allocated $1.488 billion to deploy
networks serving more than 700,000
unserved rural homes and businesses
across 45 states. The Rural Digital
Opportunity Fund represents the
Commission’s single biggest step to
close the digital divide by providing up
to $20.4 billion to connect millions
more rural homes and small businesses
to high-speed broadband networks. It
will ensure that networks stand the test
of time by prioritizing higher network
speeds and lower latency, so that those
benefitting from these networks will be
able to use tomorrow’s internet
applications as well as today’s.
II. Discussion
3. To ensure continued and rapid
deployment of broadband networks to
unserved Americans, the Commission
establishes the Rural Digital
Opportunity Fund, which will commit
up to $20.4 billion over the next decade
to support up to gigabit speed
broadband networks in rural America.
The Commission opts to allocate this
funding through a multi-round, reverse,
descending clock auction that favors
faster services with lower latency and
encourages intermodal competition in
order to ensure that the greatest possible
number of Americans will be connected
to the best possible networks, all at a
competitive cost. In light of the need to
bring service both to consumers in areas
wholly unserved by 25/3 Mbps, as well
as those living in areas partially served,
the Commission will assign funding in
two phases: Phase I will target those
areas that current data confirm are
wholly unserved; and, Phase II will
target unserved locations within areas
that data demonstrates are only partially
served, as well as any areas not won in
Phase I. By relying on a two-phase
process, the Commission can move
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13773
expeditiously to commence an auction
in 2020 for those areas it already knows
with certainty are currently unserved,
while also ensuring that other areas are
not left behind by holding a second
auction once the Commission has
identified any additional unserved
locations through improvements to its
broadband deployment data collection.
4. The Rural Digital Opportunity
Fund Phase I auction will make use of
many of the rules that made the CAF
Phase II auction a success, with some
exceptions to account for the passage of
time and other changed circumstances.
Most importantly, in addition to the
weighting of performance tiers and
latency, the Commission will assign
support in the auction’s clearing round
to the bidder with the lowest weight.
After the auction, the Commission will
require Phase I support recipients to
offer the required voice and broadband
service to all eligible homes and small
businesses within the awarded areas,
without regard to the number of
locations identified by the Connect
America Cost Model (CAM), and instead
as determined subsequently by the
Wireline Competition Bureau (the
Bureau). This approach differs from that
used in the CAF Phase II auction, which
tied the deployment and service
obligations to a specific number of
locations within awarded areas but
allowed the recipients to demonstrate
that their obligations should be reduced
(along with a corresponding reduction
in support) where there were fewer
locations than the CAM specified. As
discussed in the following, the
Commission will use its cost model and
current data to establish initial service
milestones and to monitor interim
progress, but the Commission
emphasizes that Phase I bidders will be
competing for support amounts to offer
service to all locations ultimately
identified in an area, not just to the
specific number of locations in that area
identified prior to the auction, without
adjusting awarded support amounts.
5. The Commission adopts a term of
support of 10 years for the Rural Digital
Opportunity Fund. The Commission
believes that the stability of a 10-year
term of support was partially
responsible for the robust participation
that occurred in the CAF Phase II
auction. The Commission expects that
the same principles regarding
encouraging long-term investments and
auction participation will also apply to
the Rural Digital Opportunity Fund.
Most commenters addressing this issue
agree that a 10-year term of support will
provide the certainty and stability
needed to encourage broadband
deployment in unserved and
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]]>Agencies
[Federal Register Volume 85, Number 47 (Tuesday, March 10, 2020)]
[Rules and Regulations]
[Pages 13760-13773]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2020-04746]
[[Page 13760]]
-----------------------------------------------------------------------
ENVIRONMENTAL PROTECTION AGENCY
40 CFR Part 725
[EPA-HQ-OPPT-2011-0740; FRL-9991-60]
RIN 2070-AJ65
Microorganisms; General Exemptions From Reporting Requirements;
Revisions to Recipient Organisms Eligible for Tier I and Tier II
Exemptions
AGENCY: Environmental Protection Agency (EPA).
ACTION: Final rule.
-----------------------------------------------------------------------
SUMMARY: EPA is issuing a final rule to add Trichoderma reesei (T.
reesei) strain QM6a and its derivatives and Bacillus amyloliquefaciens
(B. amyloliquefaciens) subspecies (subsp.) amyloliquefaciens to the
list of recipient microorganisms that may be used to qualify for the
Tier I and Tier II exemptions from full notification and reporting
procedures under the Toxic Substances Control Act (TSCA) for new
microorganisms that are being manufactured for introduction into
commerce. EPA received petitions to add T. reesei and B.
amyloliquefaciens to the list of microorganisms eligible for the
exemption from full notification and reporting procedures under the
TSCA for new microorganisms. Based on EPA's evaluation of these
petitions, EPA has made the determination that certain strains of both
microorganisms will not present an unreasonable risk of injury to
health or the environment when used as a recipient microorganism
provided that certain criteria for the introduced genetic material and
the physical containment conditions are met.
DATES: This final rule is effective April 9, 2020.
ADDRESSES: The docket for this action, identified by docket
identification (ID) number EPA-HQ-OPPT-2011-0740, is available at
https://www.regulations.gov or at the Office of Pollution Prevention and
Toxics Docket (OPPT Docket), Environmental Protection Agency Docket
Center (EPA/DC), West William Jefferson Clinton Bldg., Rm. 3334, 1301
Constitution Ave. NW, Washington, DC. The Public Reading Room is open
from 8:30 a.m. to 4:30 p.m., Monday through Friday, excluding legal
holidays. The telephone number for the Public Reading Room is (202)
566-1744, and the telephone number for the OPPT Docket is (202) 566-
0280. Please review the visitor instructions and additional information
about the docket available at https://www.epa.gov/dockets.
FOR FURTHER INFORMATION CONTACT:
For technical information contact: Rebecca Edelstein, Chemical
Control Division (7405M), Office of Pollution Prevention and Toxics,
Environmental Protection Agency, 1200 Pennsylvania Ave. NW, Washington,
DC 20460-0001; telephone number: (202) 564-1667; email address:
[email protected].
For general information contact: The TSCA-Hotline, ABVI-Goodwill,
422 South Clinton Ave., Rochester, NY 14620; telephone number: (202)
554-1404; email address: [email protected].
SUPPLEMENTARY INFORMATION:
I. Executive Summary
A. Does this action apply to me?
You may be potentially affected by this action if you produce,
import, process, or use either intergeneric T. reesei or intergeneric
B. amyloliquefaciens or any other eligible recipient microorganisms
listed in 40 CFR 725.420. The following list of North American
Industrial Classification System (NAICS) codes is not intended to be
exhaustive, but rather provides a guide to help readers determine
whether this document applies to them. Potentially affected entities
may include:
Basic Chemical Manufacturing (NAICS code 3251).
Pesticide, Fertilizer and other Agricultural Chemical
manufacturing (NAICS code 3253).
Other Chemical Product and Preparation Manufacturing
(NAICS code 3259).
If you have any questions regarding the applicability of this
action to a particular entity, consult the technical person listed
under FOR FURTHER INFORMATION CONTACT.
B. What is the Agency's authority for taking this action?
This action is being taken under the authority of TSCA section
5(h)(4) (15 U.S.C. 2604(h)(4)). TSCA section 5(a)(1) requires that
persons notify EPA at least 90 days before they manufacture (the term
``manufacture'' includes import under TSCA) for commercial purposes a
``new'' chemical substance, or manufacture (including import) or
process a chemical substance for a ``significant new use'' (15 U.S.C.
2604(a)(1)(B)(i)). TSCA furthermore prohibits such manufacturing or
processing from commencing until EPA has conducted a review of the
notice, made an appropriate determination on the notice, and taken such
actions as are required in association with that determination (15
U.S.C. 2604(a)(1)(B)(ii)). TSCA defines ``chemical substance'' broadly
and in terms that cover intergeneric microorganisms as well as
traditional chemical substances. Therefore, for the purposes of TSCA, a
``new microorganism'' is one that is not listed on the TSCA Chemical
Substances Inventory (TSCA Inventory) compiled under TSCA section 8(b).
TSCA section 5(h)(4) authorizes EPA, upon application and by rule,
to exempt the manufacturer of any new chemical substance from part or
all of the provisions of TSCA section 5, if EPA determines that the
manufacture, processing, distribution in commerce, use, or disposal of
the new chemical substance will not present an unreasonable risk of
injury to human health or the environment, including an unreasonable
risk to a potentially exposed or susceptible subpopulation identified
by the Administrator under the conditions of use.
C. What action is the Agency taking?
In 2012, EPA proposed to add T. reesei strain QM6a and its
derivatives (hereafter, T. reesei QM6a) and B. amyloliquefaciens
subspecies (subsp.) amyloliquefaciens to the list of recipient
microorganisms in 40 CFR 725.420 that may be used to qualify for Tier I
and Tier II exemptions from full notification and reporting procedures
under TSCA for new microorganisms that are being manufactured into
commerce. EPA is finalizing the proposal.
D. Why is the Agency taking this action?
EPA received petitions to add T. reesei and B. amyloliquefaciens to
the list of microorganisms that may be used as recipient microorganisms
in order to qualify for the exemption from full notification and
reporting procedures under TSCA for new microorganisms that are being
manufactured for introduction into commerce. EPA proposed to add
certain strains of these two microorganisms to the list of recipient
microorganisms based on EPA's preliminary determination. EPA is now
issuing a final rule that incorporates certain changes in response to
public comment.
E. What are the estimated incremental impacts of this final rule?
EPA has evaluated the potential costs of the addition of the two
microorganisms to the list of recipient microorganisms eligible for
Tier I and Tier II exemptions. The final rule is
[[Page 13761]]
expected to generate cost savings for organizations that, in the
absence of the rule, would submit Microbial Commercial Activity Notices
(MCANs) for new intergeneric T. reesei or B. amyloliquefaciens strains.
The rule will result in costs savings for both the industry and the
Agency. EPA estimates the annualized industry savings of the rule to be
approximately $260,000 per year over a ten-year period, with a 3
percent discount rate, and $252,000 per year with a 7 percent discount
rate. Annualized agency savings are approximately $178,000 per year
with a 3 percent discount rate and $173,000 per year with a 7 percent
discount rate over the ten-year period, for a total annualized savings
to society of approximately $438,000 per year with a 3 percent discount
rate and $424,000 per year with a 7 percent discount rate. The economic
analysis is available in the docket and is summarized in Unit IX. of
this final rule. Costs and benefits of adding T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens to 40 CFR 725.420 are also
discussed in Unit VIII.C.2. through 4.
II. Background
EPA received petitions to add T. reesei and B. amyloliquefaciens to
the list of recipient microorganisms at 40 CFR 725.420 that are
eligible for the regulatory exemptions applicable to new microorganisms
that are manufactured for introduction into commerce (Refs. 1-3). In
the Federal Register of September 5, 2012 (77 FR 54499) (FRL-9348-1)
(``2012 Proposed Rule'') (Ref. 4), the Agency proposed to add certain
strains of these two microorganisms to the list of recipient
microorganisms at 40 CFR 725.420 based on EPA's preliminary
determination that both of the microorganisms, with certain
limitations, meet the criteria for addition to the list--i.e., they
will not present an unreasonable risk of injury to health or the
environment provided that the other conditions of the exemptions at 40
CFR part 725, subpart G, relating to the introduced genetic material,
and the physical containment of the new microorganisms, have been met.
EPA is now issuing a final rule that incorporates certain changes made
in response to public comments received on the 2012 Proposed Rule.
These changes are described in the following paragraphs.
In the 2012 Proposed Rule, EPA proposed to restrict the exemption
for T. reesei to the T. reesei strain QM6a and its derivatives. In
addition, EPA proposed to restrict the T. reesei QM6a exemption to use
of the microorganism only under submerged standard industrial
fermentation operations used for enzyme production; as described in
this proposed rule, these conditions are typical throughout the
fermentation industry and meet the existing physical containment and
control requirements for the tiered exemptions under 40 CFR 725.422.
Any subsequent deliberate fermentation of solid plant material or
insoluble substrates with T. reesei QM6a and its derivatives as defined
at 40 CFR 725.3 could only be initiated after inactivation of the
viable T. reesei cells as delineated in 40 CFR 725.422(d), i.e., by a
procedure that has been demonstrated and documented to be effective in
reducing the viable microbial population by at least 6 logs (i.e., six
orders of magnitude).
In addition, EPA proposed to limit the exemption for B.
amyloliquefaciens to only strains of B. amyloliquefaciens that would
fall under the subspecies B. amyloliquefaciens amyloliquefaciens.
In response to comments received on its original proposal, EPA has
modified the regulatory text in 40 CFR 725.3 and 725.420 slightly to
better clarify EPA's original intent. These revisions to the regulatory
text in 40 CFR 725.3 and 725.420 merely represent a clarification of
the original proposal.
Existing regulatory requirements and exemptions for intergeneric
microorganisms are discussed in Unit III. of this proposed rule. EPA's
response to public comments received on the 2012 Proposed Rule are
provided in Unit IV. Unit V. provides EPA's evaluation of available
information on T. reesei and B. amyloliquefaciens for the criteria
delineated in 40 CFR 725.67. Physical containment and control
technologies as well as release and exposure assessments for the two
microorganisms are discussed in Unit VI. EPA's risk assessments for T.
reesei QM6a and B. amyloliquefaciens subsp. amyloliquefaciens are
summarized in Unit VII., and EPA's rationale for adding the two
microorganisms to the list of recipients eligible for exemption is
discussed in Unit VIII. EPA's Risk Assessment documents (Refs. 5 and
6), available in the public docket, provide more detailed information,
and supporting references, for EPA's evaluation of the available
information and the potential risks to health and the environment.
III. Existing EPA Regulatory Requirements and Exemption Standard
Manufacturers are required to report certain information to EPA 90
days before commencing the manufacture of intergeneric microorganisms
that are not listed on the TSCA Inventory. EPA regulations at 40 CFR
part 725 establish the mechanisms for reporting this information. TSCA
prohibits such manufacturing or processing from commencing until EPA
has conducted a review of the notice, made an appropriate determination
on the notice, and taken such actions as are required in association
with that determination (15 U.S.C. 2604(a)(1)(B)(ii)).
Any manufacturer of a living intergeneric microorganism who is
required to report under TSCA section 5 must file a MCAN with EPA,
unless the activity is eligible for one of the specific exemptions.
Section 5(h)(4) authorizes EPA, by rule and upon request, to exempt
manufacturers from these requirements if the Administrator determines
that the manufacture, processing, distribution in commerce, use or
disposal of the chemical substance ``will not present an unreasonable
risk of injury to health or the environment, including an unreasonable
risk to a potentially exposed or susceptible subpopulation identified
by the Administrator under the conditions of use.'' TSCA section 3(4)
defines ``conditions of use'' to mean ``the circumstances, as
determined by the Administrator, under which a chemical substance is
intended, known or reasonably foreseen to be manufactured, processed,
distributed in commerce, used, or disposed of.'' TSCA section 3(12)
defines ``potentially exposed or susceptible subpopulation'' to mean
``a group of individuals within the general population. . .who, due to
either greater susceptibility or greater exposure, may be at greater
risk than the general population of adverse health effects from
exposure to a chemical substance or mixture, such as infants, children,
pregnant women, workers, or the elderly.'' 15 U.S.C. 2601 et seq. The
general procedures for filing MCANs are described in 40 CFR part 725,
subpart B.
EPA regulations establish two exemptions for new microorganisms,
after the research and development stage, which are being manufactured
for introduction into commerce: Tier I and Tier II exemptions.
Under the Tier I exemption, if certain criteria are met,
manufacturers are required to notify EPA 10 days prior to manufacturing
a new microorganism that qualifies for this exemption, and to keep
certain records. 40 CFR 725.400. To qualify for the Tier I exemption, a
manufacturer must use one of the recipient organisms listed in 40 CFR
725.420, and must implement specific physical containment and control
technologies listed in 40 CFR 725.422. In addition, the genetic
material
[[Page 13762]]
introduced into the recipient microorganism must be well-characterized,
limited in size, poorly mobilizable, and free of certain sequences. 40
CFR 725.421.
A manufacturer who meets the conditions of the Tier I exemption may
modify the specified containment restrictions or level of inactivation
but must submit a Tier II exemption notification 40 CFR 725.428. The
Tier II exemption requires manufacturers to submit an abbreviated
notification describing the modified containment and provides for a 45-
day period during which EPA would review the proposed containment. 40
CFR 725.450 and 725.470. The manufacturer may not proceed under this
exemption until EPA approves the exemption. 40 CFR 725.470.
EPA established a petition process at 40 CFR 725.67 for the public
to propose additional microorganisms for the tiered exemptions. EPA's
regulations at 40 CFR 725.67 direct petitioners to submit information
to demonstrate that the activities affected by the requested exemption
meet the requirements of TSCA section 5(h)(4), i.e. ``will not present
an unreasonable risk of injury to health or the environment, including
an unreasonable risk to a potentially exposed or susceptible
subpopulation identified by the Administrator under the conditions of
use.'' 15 U.S.C. 2604(h)(4). In addition, a petitioner is responsible
for providing supporting information for this determination in four
general categories:
1. The effects of the new microorganism on health and the
environment.
2. The magnitude of exposure of human beings and the environment
to the new microorganism.
3. The benefits of the new microorganism for various uses and
the availability of substitutes for such uses.
4. The reasonably ascertainable economic consequences of
granting or denying the petition, including effects on the national
economy, small business, and technological innovation.
The regulations at 40 CFR 725.67 specify that when applying to list
a recipient microorganism for the tiered exemption under 40 CFR
725.420, petitioners should include information addressing six
specified criteria, which EPA will use to evaluate the microorganism
for listing. 40 CFR 725.67(a)(3)(iii). The six criteria are:
1. Identification and classification of the microorganism using
available genotypic and phenotypic information.
2. Information to evaluate the relationship of the microorganism
to any other closely related microorganisms which have a potential
for adverse effects on health or the environment.
3. A history of safe commercial use for the microorganism.
4. Commercial uses indicating that the microorganism products
might be subject to TSCA.
5. Studies which indicate the potential for the microorganism to
cause adverse effects to health or the environment.
6. Studies which indicate the survival characteristics of the
microorganism in the environment.
IV. Response to Public Comments on the 2012 Proposed Rule
The Agency received three comments on the 2012 Proposed Rule (Ref.
4). One comment, from an anonymous submitter (Ref. 7), concerned mold
problems in rental housing and thus was not relevant to the proposed
rule. A second comment, from an individual (Ref. 8), supported the
proposed rule.
The third comment was a joint set of comments from the
Biotechnology Industry Organization (BIO) and the Enzyme Technical
Association (ETA) (Ref. 9). While generally supportive of the proposed
rule, BIO/ETA raised three important issues with respect to EPA's
proposed rule.
First, BIO/ETA expressed concern that the proposed wording in
section 725.420(k), that reads ``Trichoderma reesei strain QM6a used
only in . . .'' does not accurately reflect the range of T. reesei
strain QM6a microorganisms currently being used in standard industrial
fermentations. BIO/ETA requested that the phrase be reworded as
``Trichoderma reesei strain QM6a and its derivatives used only in . .
.'' EPA agrees that the commenter's suggested language more accurately
reflects the Agency's original intent. EPA did not originally intend to
restrict the exemption to the naturally occurring QM6a isolate. Most of
the strains of T. reesei currently used in industrial production are
not the naturally occurring QM6a isolate, but are strains derived from
QM6a that have been modified by physical or chemical mutagenesis to
obtain microorganisms with improved enzyme-producing abilities.
Accordingly, EPA has adopted the commenter's suggested revision to
clarify that the exemption applies not only to the naturally occurring
strain, but also to any strain derived from the naturally occurring
QM6a.
Second, BIO/ETA expressed concern that the proposed regulation was
too broadly worded and as drafted would not clearly distinguish between
standard industrial fermentation operations used to produce enzymes,
and fermentation operations conducted for other purposes. Specifically,
the commenter raised concern that the inclusion of an unqualified
restriction in proposed 40 CFR 725.420(k) that ``no solid plant
material or insoluble substrate is present in the fermentation broth''
would prohibit the use of T. reesei in submerged standard industrial
fermentation operations used for enzyme production. Enzyme production
is the first phase of some industrial applications such as cellulosic
ethanol production where the first fermentation is to grow the
microorganism to produce enzymes, followed by another fermentation of
pretreated plant biomass for conversion of the cellulose and
hemicellulose to simple sugars (i.e., saccharification), followed by a
third fermentation of the sugars to ethanol by yeast or another
ethanologen. As part of the process of growing the microbes for enzyme
production by T. reesei QM6a and its derivatives, nutrients need to be
available, including those from plant materials such as soy or corn,
which may contain insoluble components. The second fermentation
operation of saccharification of plant biomass may occur only after the
T. reesei microorganism has been inactivated. The use of nutrients
supplied by plant material (e.g., soy meal, corn steep liquor) in the
first fermentation for enzyme production has a long history of safe
use.
To address this issue, the commenter suggested revising the
regulatory text to ensure that the typical industry practice of
supplying nutrients in the form of solid plant materials during the
initial enzyme fermentation would fall within the scope of the proposed
exemption. EPA agrees and is therefore changing the regulatory text to
allow the use of solid plant material in the enzyme fermentation step.
Under the final regulatory text, the use of the conventional
fermentation ingredients from solid plant material--for example, soy or
corn meal and other insoluble fermentation ingredients from corn or soy
which contain insoluble components--is allowed when used specifically
to provide nutrients for growth of the microorganism during standard
enzyme fermentation as described in part 1 of the definition at 40 CFR
725.3.
The commenter further suggested adding text to clarify that the
requirement to inactivate the organism applies prior to ``subsequent
fermentation operations, and not to the initial enzyme production
stage.'' EPA agrees that the commenter has identified a reasonable
basis for concern with respect to the proposed regulatory text. EPA
acknowledges that nutrients for microbial growth in submerged standard
industrial fermentation during the initial enzyme production phase of
the
[[Page 13763]]
fermentation operation may be supplied by soybean meal, corn steep
liquor, or other plant-derived materials that may contain insoluble
substrates. The use of such plant materials as nutrient sources for
microbial growth in submerged standard industrial fermentation
operations used for enzyme production is a standard industry practice
with a long history of safe use, and it does not result in the
production of secondary toxic metabolites such as paracelsin because
the fermentations involve the logarithmic growth of the cells in the
presence of optimal concentrations of carbon and nitrogen and other
nutrients (see Unit V. for more detail on paracelsin). EPA did not
originally intend to preclude such operations and agrees that revision
to the regulatory text is warranted to clarify that solid plant
material can be used to provide nutrients for growth of the
microorganism during submerged standard enzyme fermentation operations.
However, EPA continues to have concern about the potential for the
production of paracelsin during the second fermentation phase of
cellulosic ethanol production, i.e., the saccharification of the
pretreated plant biomass, because of the presence of solid surfaces and
an excess of carbon substrate with live T. reesei QM6a (and its
derivatives) cells. Therefore, EPA is retaining the requirement that
fermentation operations subsequent to the enzyme production
fermentation phase may only be initiated after inactivation of the
viable T. reesei cells as delineated in 40 CFR 725.422(d) (i.e., by a
procedure that has been demonstrated and documented to be effective in
reducing the viable microbial population by at least 6 logs).
Inactivation of T. reesei QM6a prior to a subsequent or secondary
fermentation that may contain solid plant material or insoluble
substrates (as defined at 40 CFR 725.3) avoids the potential for
production of paracelsin.
BIO/ETA also commented that paracelsin may be produced under non-
standard conditions of fermentation, such as ``surface fermentation
media with large concentrations of biomass,'' and requested that EPA
revise the rule to reflect this. EPA interprets this comment to mean
``surface fermentation media with large concentrations of biomass'' is
the only condition under which paracelsin can be produced and that BIO/
ETA is requesting that the rule be amended accordingly. EPA agrees that
paracelsin may be produced under non-standard conditions of
fermentation, such as surface fermentation with large concentrations of
biomass. However, available scientific literature indicates that
paracelsin may also be produced under certain other fermentation
conditions. Scientific literature suggests that surface fermentation is
synonymous with solid-state fermentation where microorganisms are grown
on the surface of a solid support that is not submerged. While it is
likely that the potential for paracelsin production is greater with
solid-state/surface fermentation, the production of peptaibols (of
which paracelsin is one) by Trichoderma species has been shown to occur
even in liquid broth culture in the presence of plant material or
insoluble substrates in laboratory studies. Thus, paracelsin production
potentially may be produced in fermentation broth amended with plant
material providing excess carbon. Therefore, EPA is not amending the
rule to indicate that the only conditions in which paracelsin
potentially may be produced are with surface fermentations with large
concentrations of biomass.
V. EPA's Evaluation of Available Information on T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens for the Criteria Delineated
Pursuant to 40 CFR 725.67, Genencor International, Inc.,
(subsequently supported by the Enzyme Technical Association (ETA)) and
Novozymes North America, Inc., submitted Letters of Application to EPA
requesting that T. reesei and B. amyloliquefaciens (Refs. 1 and 2) be
added to 40 CFR 725.420 as candidate recipient microorganisms for the
tiered exemptions. The letters of application provided information that
the submitters believed demonstrate that activities affected by the
requested exemptions would not present an unreasonable risk of injury
to health or the environment. Information regarding the criteria
specified in 40 CFR 725.67(a)(2) and 725.67(a)(3)(iii) were addressed
in these letters of application to list T. reesei and B.
amyloliquefaciens as recipient microorganisms under 40 CFR 725.420.
EPA has made the determination based on the information provided in
the Letters of Application (Refs. 1 and 2), supplemental information
provided by ETA (Refs. 10 and 11), and other information available to
EPA that T. reesei QM6a, with certain restrictions, and B.
amyloliquefaciens subsp. amyloliquefaciens will not present an
unreasonable risk of injury to health or the environment, including an
unreasonable risk to a potentially exposed or susceptible
subpopulation, when used as recipient microorganisms provided that: (a)
The existing criteria for the introduced genetic material listed in 40
CFR 725.422 are met, and (b) the physical containment and control
technologies criteria listed at 40 CFR 725.422 are met. In making this
determination, EPA identified workers as a potentially exposed or
susceptible subpopulation to the substances under the conditions of use
and concluded that, with the limitations described above, the
substances will not present an unreasonable risk of injury to health or
the environment. EPA's Risk Assessments for these two microorganisms
(Refs. 5 and 6) are available in the docket.
This unit presents a summary of EPA's evaluation of the available
information pertinent to the six criteria delineated in 40 CFR
725.67(a)(3)(iii) for both microorganisms.
A. Evaluation of Available Information Relevant to the Criteria for T.
reesei QM6a as a Recipient Microorganism with Specified Conditions of
Growth
1. Identification and classification of the microorganism using
available genotypic and phenotypic information.
T. reesei is a hypercellulolytic fungus originally isolated in the
Solomon Islands in 1944. T. reesei was found on deteriorating military
fabrics such as tents and clothing. This isolate, designated as QM6a,
was initially named Trichoderma viride. Approximately 20 years later,
QM6a was re-classified as Trichoderma reesei.
T. reesei is the species name given to the anamorphic form (this
form reproduces asexually) of the fungus whose teleomorphic form (this
form reproduces sexually) is now understood to be Hypocrea jecorina.
Recent taxonomic studies have shown that the species T. reesei
consists only of this single isolate QM6a and its derivatives. Many
other strains called T. reesei isolated elsewhere have now been
proposed as belonging to a newly named species, T. parareesei, based on
differences in habitat, sporulation, and metabolic versatility. T.
reesei has been shown to belong to a single species now referred to as
H. jecorina/T. reesei (QM6a) which reflects its relationship to its
teleomorph H. jecorina. The only anamorphic strains within the species
H. jecorina/T. reesei are those of QM6a and its derivatives. The
petition to add T. reesei to the list of microorganisms at 40 CFR
725.420 requested that EPA include all strains of T. reesei. However,
given these recent taxonomic publications, all fungal strains correctly
named T. reesei are, by definition, QM6a or a derivative.
[[Page 13764]]
Adequate genotypic and phenotypic information is available for
classification of T. reesei QM6a and its derivatives. The American Type
Culture Collection (ATCC) designation for this original strain of T.
reesei QM6a is ATCC 13631.
2. Information to evaluate the relationship of the microorganism to
any other closely related microorganisms that have a potential for
adverse effects on health or the environment.
Closely related members of section Longibrachiatum do not have a
potential for adverse effects; other less closely related Trichoderma
species have a potential to cause adverse effects as pathogens of
commercially produced mushrooms. These less closely related species
include various species of the Harzianum clade, T. aggressivum, T.
pleuotrophilum, and T. fulvidum that are responsible for significant
loss of the mushroom crops of Agaricus bisporus and Pleurotus
ostreatus.
T. reesei/H. jecorina can be distinguished from other Trichoderma
species by a comprehensive approach employing criteria of the
Genealogical Concordance Phylogenetic Species Recognition (GCPSR)
concept, which commonly requires the use of genealogies of three or
four genes, not just the sequences of spacer regions as previously
utilized for identification. Use of the GCPSR protocol would separate
T. reesei (sensu lato) from the opportunistic pathogens within the
section Longibrachiatum, including T. longibrachiatum and T.
citrinoviride/H. schweinitzii, as well as the mold disease pathogens of
mushrooms.
3. A history of safe commercial use for the microorganism.
T. reesei QM6a has a long history of safe use producing a variety
of commercial enzymes. T. reesei QM6a cellulases, beta-glucanases, and
xylanases are used by the animal feed, baking, beverages, textile
processing, detergent, pulp and paper, industrial chemicals, and
biofuels industries.
For industrial enzyme production, T. reesei is generally grown in a
closed, submerged standard industrial fermentation system. In submerged
standard industrial fermentation operations used for enzyme production,
growth of the microorganism occurs beneath the surface of the liquid
growth medium. As described in this unit, this type of fermentation
system appears to be typical throughout the industry, based on EPA's
review of MCAN submissions over the years.
Under this type of fermentation system, the fermentation broth is a
defined mixture of carbon and nitrogen sources, some of which may be
supplied from plant material or soluble substrates (e.g., soy meal,
corn steep liquor), minerals, salts, and other nutrients, is maintained
at optimal pH and temperature, and is typically aerated and mixed.
These conditions support the active growth and productivity of the
organisms for enzyme production. Submerged standard industrial
fermentation operations used for enzyme production systems reduce the
potential for exposure of workers to the production organism and
fermentation broth aerosols, reduce the potential for contamination of
the culture and make the collection of extracellular enzymes simpler
and less costly. The fermentation process is terminated before the T.
reesei QM6a organisms go into the stationary growth phase (i.e., before
secondary metabolism begins). At the end of the fermentation process,
the production organisms are separated from the fermentation broth and
inactivated.
Several enzymes produced by T. reesei QM6a have Generally
Recognized as Safe (GRAS) status with the Food and Drug Administration
(FDA) or FDA had no questions about the GRAS conclusions about them
contained in GRAS submissions to FDA. This supports the Agency's
conclusion that commercial use of T. reesei QM6a and its derivatives as
a recipient microorganism for commercial enzyme production will not
present an unreasonable risk of injury to health or the environment. T.
reesei QM6a enzymes used in foods that have been granted GRAS status or
for whose claimed GRAS status FDA had no questions include cellulase,
hemicellulase, transglucosidase, pectin lyase, acid fungal protease,
and a chymosin enzyme preparation. Data supporting the GRAS notices
included the results of pathogenicity tests for the T. reesei QM6a
production organisms and toxicity tests for the enzyme products. The
data showed that the production strains are not pathogenic and did not
produce toxins during enzyme fermentation.
4. Commercial uses indicating that the microorganism products might
be subject to TSCA.
EPA has reviewed 48 MCANs involving intergeneric T. reesei
production organisms used to manufacture a number of industrial
enzymes, including amylases, glucosidases, proteases, phytase, laccase,
and numerous cellulolytic enzyme preparations. Amylases and
glucosidases are used for the breakdown of starch into sugars and have
been used in laundry detergents and in textile processing. More
recently, industrial enzymes produced by T. reesei have been produced
for corn and cellulosic ethanol production. T. reesei produces numerous
cellulases and hemicellulases that are efficient in degrading plant
biomass. Intergeneric T. reesei strains could also be used to
manufacture industrial chemicals other than enzymes such as surfactants
or specialty chemicals. More detailed information on MCANs submitted to
EPA can be viewed on EPA's TSCA Biotechnology Program web page: https://www.epa.gov/regulation-biotechnology-under-tsca-and-fifra/overview-biotechnology-under-tsca.
5. Studies which indicate the potential for the microorganism to
cause adverse effects to health or the environment.
a. Human health hazards -- i. Pathogenicity. T. reesei QM6a is not
pathogenic to humans. Due to its long history of use for production of
enzymes used in food applications, the potential for the fungus and its
products to be pathogenic or toxic to humans has been evaluated
numerous times. Various studies have been conducted assessing T. reesei
QM6a's pathogenic potential in healthy and immunocompromised laboratory
animals. With the exception of one study where a high inoculum of
intravenous (iv) and intraperitoneal (ip) injection of spores in
immunocompromised mice resulted in pathogenic effects, studies have
demonstrated a lack of pathogenicity of T. reesei QM6a. Numerous
pathogenicity studies have been conducted as part of GRAS notices to
FDA for several different enzymes used in the food industry. Studies
using injection of T. reesei QM6a in rats, using both healthy and
immunosuppressed rats, and using ip injection of viable and heat-killed
cells of T. reesei QM6a in rats have all demonstrated a lack of
potential pathogenicity to humans.
T. reesei QM6A is not known to possess any virulence factors
associated with colonization or disease such as adherence factors,
penetration factors, necrotic factors, toxins, or the ability to grow
at human body temperature, 37 [deg]C. There are no reports of harmful
effects associated with the use of or exposure to T. reesei QM6A
strains, even after decades of commercial use for enzyme production.
The body of evidence indicates that T. reesei QM6A does not pose
concerns regarding human pathogenicity.
ii. Toxicity. Available data indicate that T. reesei QM6a strains
used in submerged standard industrial fermentation operations used for
enzyme production do not present
[[Page 13765]]
human toxicity concerns. A number of studies have been conducted
assessing the potential for T. reesei QM6a to produce toxins during
submerged standard industrial fermentation operations used for enzyme
production for food, pharmaceutical, or industrial uses. A cellulase
enzyme known as celluclast produced by T. reesei QM6a has been tested
for general oral toxicity and inhalation toxicity. Acute oral toxicity
studies conducted in mice, rats, and dogs showed that T. reesei QM6a
cellulase was not toxic to any of the test animals. Subchronic toxicity
studies showed no evidence of systemic effects in dogs or rats.
Additional toxicity studies have been conducted on other enzymes
produced by T. reesei QM6a, the results of which have been presented in
various GRAS petitions. Acute oral toxicity tests on two endoglucanases
and a glucoamylase showed a lack of toxins. Subchronic feeding studies
conducted on a cellulase, two xylanases, two endoglucanases, a
protease, and a glucoamylase also showed a lack of toxicity in rats.
Under typical industry practice, industrial fermentations of T.
reesei QM6a for enzymes to be used in food are routinely checked by the
enzyme producers to confirm the absence of antibiotic activity and
toxins (Ref. 12). Relying on the data that show T. reesei QM6a has a
long history of safe use in the production of food enzymes, EPA has
concluded that strains used industrially would not be expected to
produce these toxins under the conditions of submerged standard
industrial fermentation used for enzyme production.
iii. Mycotoxins and other secondary metabolites. The only health
concern associated with T. reesei QM6a is its ability to produce a
peptaibol secondary metabolite called paracelsin. Peptaibols are small
linear peptides of 1,000-2,000 daltons characterized by a high content
of the non-proteinogenic amino acid [alpha]-amino-isobutyric acid
(Aib), with an N-terminus that is typically acetylated, and a C-
terminus that is linked to an amino alcohol, which is usually
phenylalaninol, or sometimes valinol, leucinol, isoleucinol, or
tryptophanol. Peptaibols are associated with a wide variety of
biological activities and have antifungal, antibacterial, sometimes
antiviral, antiparasitic, and neurotoxic activity. Paracelsin has been
shown to damage mammalian cells such as human erythrocytes with an in
vitro hemolytic activity of C50 = 3.7 x 10\-5\ mole/liter
(mol/L) (Ref. 5).
Paracelsin has not been detected in the use of T. reesei QM6a under
the submerged standard industrial fermentation operations used for
enzyme production, and numerous toxicity studies on enzyme products of
T. reesei QM6a have demonstrated a lack of toxicity to laboratory
animals. EPA therefore expects that paracelsin production would be of
insignificant concern, provided the microorganisms are produced with
submerged standard industrial fermentation operations used for enzyme
production as described at 40 CFR 725.3.
Under other conditions of fermentation, for example with the
deliberate fermentation of cellulosic biomass for saccharification of
plant material or extended fermentation, paracelsin may be produced
(Ref. 5). Neither the information submitted with the petition, nor the
information that is otherwise available is sufficient to allow EPA to
determine the extent of paracelsin formation under these non-standard
conditions. Consequently, EPA is unable to determine whether the use of
the microbe under conditions other than submerged standard industrial
fermentation operations used for enzyme production (i.e., specific
conditions under which paracelsin is not expected to be formed) will
not pose an unreasonable risk to human health and/or the environment
(Ref. 5).
b. Environmental hazards--i. Hazards to animals. T. reesei QM6a is
not pathogenic to domesticated animals or wildlife. However, the
secondary metabolite paracelsin has been shown to exhibit toxicity to
aquatic species. A 24-hr exposure of paracelsin to Artemia salina
(brine shrimp) resulted in a lethal concentration of 50%
(LC50) of 21.26 micromoles ([micro]M) (40.84 micrograms per
milliliter ([micro]g/ml)) which decreased to 9.66 [micro]M (18.56
[micro]g/ml) with a 36-hr exposure. With Daphnia magna, paracelsin was
found to be moderately toxic, with an LC50 of 7.70 [micro]M
(14.79 [micro]g/ml) with a 24-hr exposure, and 5.60 [micro]M (10.76
[micro]g/ml) with a 36-hr exposure.
ii. Hazards to plants. T. reesei QM6a is not a pathogen of plants.
Although it is capable of degrading cellulose and hemicellulose due to
the copious quantities of the enzymes it can produce, it cannot be a
primary colonizer on plant tissue. Genetic studies have shown that T.
reesei QM6a does not contain any genes for ligninases, required for
initial breakdown of plant material. This species is known as a wood
rot fungus, but it apparently attacks only decaying plant material, not
live plants.
iii. Effects on other organisms. Peptaibols are toxic to Gram-
positive bacteria and various fungi. The inhibitory action of
peptaibols on various fungi is the reason that many species of
Trichoderma are used as biocontrol agents of plant pathogenic fungi.
The peptaibol produced by T. reesei, QM6a paracelsin, has been shown to
be inhibitory to one particular fungus, Phoma destructiva.
Some species of Trichoderma, specifically T. aggressivum, T.
pleuotrophilum, and T. fulvidum are pathogens of mushrooms. However, T.
reesei QM6a is not a pathogen of mushrooms.
6. Studies which indicate the survival characteristics of the
microorganism in the environment. The species T. reesei is known only
from the single original isolate QM6a from the Solomon Islands.
Therefore, there is little information on its prevalence or behavior in
the environment. Microcosm studies have been conducted that suggest it
would survive in the environment in the plant rhizosphere and in bulk
soils if inadvertently released.
Although T. reesei was originally isolated from a tropical climatic
region, it would be expected to persist in soils for extended periods
of time, even after cold temperatures.
B. Evaluation of Available Information Relevant to the Criteria for B.
amyloliquefaciens as a Recipient Microorganism
1. Identification and classification of the microorganism using
available genotypic and phenotypic information.
B. amyloliquefaciens was initially proposed as a unique species in
1943. The name B. amyloliquefaciens lost standing when it was not
included on the Approved List of Bacterial Names with Standing in
Nomenclature in 1980. Since classical phenotypic tests could not
differentiate it as a unique species from Bacillus subtilis, it was
regarded as a subspecies of B. subtilis for several decades. However,
molecular evidence from subsequent studies led to the conclusion that
B. amyloliquefaciens did indeed deserve independent status. The DNA
homology between B. subtilis and B. amyloliquefaciens is only about
15%. In addition, there were several phenotypic properties that
differed between the two species. Chemotaxonomic studies revealed
additional capability of separating strains of B. amyloliquefaciens
from the other related species, Bacillus subtilis, Bacillus
licheniformis, and Bacillus pumilus. The species has remained within
the genus Bacillus sensu stricto since it was last established as a
separate species.
Recently, it has been proposed that there are two subspecies within
the species B. amyloliquefaciens, B.
[[Page 13766]]
amyloliquefaciens subsp. amyloliquefaciens and B. amyloliquefaciens
subsp. plantarum. The former subspecies includes the type strain and
likely most, if not all, of the industrial strains of B.
amyloliquefaciens used for enzyme production. The latter subspecies
consists of plant-associated strains used as biocontrol agents due to
the production of several antifungal lipopeptide and antibacterial
polyketide toxins. This exemption is restricted to the subspecies B.
amyloliquefaciens subsp. amyloliquefaciens which contains the
industrial strains used for enzyme production. Adequate genotypic and
phenotypic information is available to accurately identify B.
amyloliquefaciens subsp. amyloliquefaciens.
2. Information to evaluate the relationship of the microorganism to
any other closely related microorganisms which have a potential for
adverse effects on health or the environment.
There are several species in the genus Bacillus that are known
pathogens. These include Bacillus anthracis, which is pathogenic to
humans and other animals, and Bacillus cereus, which is a common cause
of food poisoning. Bacillus thuringiensis, Bacillus larvae, Bacillus
lentimorbus, Bacillus popilliae, and some strains of Bacillus
sphaericus are pathogenic or toxigenic to certain insects. The new
subspecies Bacillus amyloliquefaciens subsp. plantarum has been shown
to exhibit toxicity mainly to plant pathogenic fungi but can also be
cytotoxic to mammalian cells. It is possible, using polyphasic
approaches, to differentiate between B. amyloliquefaciens subsp.
amyloliquefaciens and these other species and subspecies that have the
potential to adversely affect humans or other organisms. B.
amyloliquefaciens can be distinguished from the very similar Bacillus
subtilis by a few phenotypic traits and DNA dissimilarity.
3. A history of safe commercial use for the microorganism.
B. amyloliquefaciens subsp. amyloliquefaciens has been used to
produce commercial enzymes for more than 50 years. It produces
carbohydrases, proteases, nucleases, xylanases, and phosphatases that
have applications in the food, brewing, distilling, and textile
industries.
For commercial enzyme production, B. amyloliquefaciens subsp.
amyloliquefaciens is grown in a closed submerged fermentation. In
submerged fermentation, growth of the microorganism occurs beneath the
surface of the liquid growth medium. The fermentation broth is a
defined mixture of carbon and nitrogen sources, minerals, salts, and
other nutrients that is maintained at optimal pH and temperature. These
conditions support the active growth and productivity of the organisms.
Submerged fermentation systems reduce the potential for exposure of
workers to the production organism and fermentation broth aerosols,
reduce the potential for contamination of the culture, and make the
collection of extracellular enzyme simpler and less costly. The
fermentation process is terminated before the B. amyloliquefaciens
subsp. amyloliquefaciens organisms enter the stationary growth phase,
and the production organisms are separated from the fermentation broth
and inactivated. The enzyme preparation may also be subjected to other
purification processes.
B. amyloliquefaciens subsp. amyloliquefaciens has a long history of
safe use for enzyme production in food and industrial applications with
no incidences associated with human pathogenicity. In response to a
petition from the ETA, FDA affirmed that carbohydrase enzyme
preparations and protease enzyme preparations derived from either
Bacillus subtilis or Bacillus amyloliquefaciens are GRAS for use as
direct food ingredients. The European Food Safety Authority (EFSA) has
put B. amyloliquefaciens on their list of bacteria that have a
``qualified presumption of safety'' because of a long history of
apparent safe use in food and feed production. However, it was put on
the list with a qualifier that only strains of B. amyloliquefaciens
that do not have toxigenic potential be used.
One strain of B. amyloliquefaciens has been used as a biopesticide.
A naturally occurring strain of B. amyloliquefaciens subsp. plantarum
was registered in 2000 as a biopesticide active ingredient under the
Federal Insecticide, Fungicide, and Rodenticide Act. It can only be
used on certain ornamental, non-food plants in greenhouses and other
closed structures.
4. Commercial uses indicating that the microorganism products might
be subject to TSCA.
It is expected that intergeneric strains of B. amyloliquefaciens
subsp. amyloliquefaciens would be used to produce enzymes and to
manufacture other industrial chemicals subject to TSCA. Many enzymes
produced by B. amyloliquefaciens, particularly [alpha]-amylase, are
used in laundry detergents and in textile processing. B.
amyloliquefaciens also makes a surfactant known as surfactin which
functions as an antibiotic.
5. Studies which indicate the potential for the microorganism to
cause adverse effects to health or the environment.
a. Human health hazards-- i. Pathogenicity. B. amyloliquefaciens is
not pathogenic to humans. There are no reports in the literature
associating B. amyloliquefaciens with infection or disease in humans.
B. amyloliquefaciens has been categorized as a Biosafety Level 1(BSL1)
microorganism by the Centers for Disease Control and Prevention (CDC).
BSL1 microorganisms are well-characterized agents not known to
consistently cause disease in immunocompetent adult humans, and which
present minimal potential hazard to laboratory personnel and the
environment. Animal toxicity studies were performed with B.
amyloliquefaciens strain FZB24 to support its registration as a
biopesticide. Tests for acute oral toxicity/pathogenicity, acute
pulmonary toxicity/pathogenicity, and acute injection toxicity/
pathogenicity showed little to no adverse effects, which indicated low
mammalian toxicity and a lack of pathogenicity/infectivity.
ii. Toxins and other secondary metabolites. Although another
species in the genus Bacillus, B. cereus, has the potential to produce
food poisoning toxins which cause both emetic and diarrheal syndromes,
and a variety of local and systemic infections, the risk of food-borne
disease caused by bacilli other than B. cereus is generally considered
to be negligible because usually only B. cereus has the genes that
encode food poisoning toxins. Industrial strains of Bacillus species
belonging to the Bacillus subtilis group, which includes B.
amyloliquefaciens, do not express B. cereus toxins. In addition, there
are no reported cases of food poisoning associated with B.
amyloliquefaciens.
Some strains of B. amyloliquefaciens have been shown to produce
bioactive cyclic lipopeptide metabolites such as iturin, surfactin,
fengycin, and bacillomycin D. These are cyclical lipoprotein
biosurfactants produced by non-ribosomal peptide synthesis. They have a
low mammalian toxicity as demonstrated by a lethal dose of 50%
(LD50) of >2,500 milligram/kilogram (mg/kg) in an acute
toxicity test of surfactin C, and a no observed adverse effect level of
500 mg/kg-day in a repeat dose oral gavage study. Some strains of B.
amyloliquefaciens may also produce the polyketide toxins macrolactin,
bacillanene, and difficidin. B. amyloliquefaciens also produces the
protein toxin barnase and the antifungal protein baciamin.
[[Page 13767]]
There are reports of the isolation of B. amyloliquefaciens from
water-damaged buildings in which occupants were suffering ill health
symptoms. Extracts from biomass of isolated strains of Bacillus
exhibiting antifungal properties were assessed for toxicity endpoints.
All of the isolated B. cereus and B. amyloliquefaciens strains studied
showed cytotoxicity as evidenced by inhibition of boar spermatozoa
motility; however, the B. amyloliquefaciens strains affected boar
spermatozoa differently from the indoor B. cereus isolates and the
reference food-poisoning strain.
The isolation of cytotoxic strains of B. amyloliquefaciens from
water-damaged buildings is of little concern in relation to the
exemption of B. amyloliquefaciens subsp. amyloliquefaciens. It is
important to note that the Bacillus amyloliquefaciens strains studied
in water-damaged buildings were specifically selected for further study
because the isolates exhibited antifungal activity. Some of the
secondary metabolites produced by these strains of B. amyloliquefaciens
also exhibited cytotoxicity to mammalian cells (i.e., boar
spermatozoa). However, industrial strains of B. amyloliquefaciens that
are classified as B. amyloliquefaciens subsp. amyloliquefaciens have
been shown not to produce most, if not all, of the antifungal and
antibacterial lipopeptides and polyketides produced by the biocontrol-
type strains. The genome of the type strain of B. amyloliquefaciens DSM
7\T\ (now B. amyloliquefaciens subsp. amyloliquefaciens) is very
similar to the genome of the biocontrol strain FZB42 (B.
amyloliquefaciens subsp. plantarum). However, the latter subspecies had
genomic islands carrying prophage sequences, transposases, integrases,
and recombinases that the DSM 7\T\ type strain did not have. The DSM
7\T\ type strain was shown to have a diminished capacity to non-
ribosomally synthesize secondary metabolites with antifungal and
antibacterial activities. The DSM 7\T\ type strain could not produce
the polyketides difficidin or macrolantin, and could not produce
lipopeptide such as iturin, macrolantin, and other compounds except for
the compound surfactin.
Although there are isolated reports of toxin production in several
antifungal, environmental isolates of B. amyloliquefaciens, the larger
body of studies available on the safety and toxicity of B.
amyloliquefaciens strains used industrially for enzyme production (Ref.
6) indicate that these strains are safe and non-toxic. For example, the
industrial strains of B. amyloliquefaciens, Bacillus subtilis, and
Bacillus licheniformis used for large-scale enzyme production did not
exhibit any cytotoxicity in Chinese hamster ovary tests. In Europe, the
toxicity of two strains of B. amyloliquefaciens used in the production
of [alpha]-amylase and bacillolysin was assessed by EFSA's Scientific
Panel on Additives and Products or Substances used in Animal Feed. The
panel concluded that the B. amyloliquefaciens production strains
DSM9553 and DSM9554, when used as a source of extracellular enzyme, do
not present a toxigenic risk. Given its widespread distribution in the
environment, its long history of safe use in industrial fermentation,
the absence of reports on pathogenicity to humans, and the limited
reports of cytotoxicity, EPA concludes that the use of B.
amyloliquefaciens in fermentation facilities for production of enzymes
or specialty chemicals does not present a human health concern.
b. Environmental hazards-- i. Hazards to animals. There are no
reports suggesting that B. amyloliquefaciens is pathogenic to
domesticated animals or wildlife. The cytotoxicity of antifungal
secondary metabolites to mammalian cells by biocontrol strains of B.
amyloliquefaciens subsp. plantarum is discussed in this Unit.
ii. Hazards to plants. B. amyloliquefaciens is not pathogenic to
plants. The plant-associated strains of B. amyloliquefaciens are
beneficial to plants because they inhibit the growth of fungal plant
pathogens. Antifungal and antibacterial secondary metabolites produced
by strains of B. amyloliquefaciens such as iturins, surfactins,
fengycin, bacillomycins, and azalomycin have been shown to inhibit the
growth of Rhizoctonia solani, Xanthomonas campestris pv. campestris,
Alternaria brassicae, Botyris cinerea, Leptosphaeria maculans,
Verticillium longisporum, Pythium ultimatum, Aspergillus spp., Fusarium
spp., Bipolaris sorokiniana, and Fusarium oxysporum.
In addition to producing antifungal and antibacterial compounds, B.
amyloliquefaciens is known as a plant growth-promoting rhizobacterium,
and some of the biological control strains of B. amyloliquefaciens were
shown to produce the phytohormone indole-3-acetic acid.
6. Studies which indicate the survival characteristics of the
microorganism in the environment.
Several studies assessing the survival of B. amyloliquefaciens are
available in the public literature and are described in EPA's Risk
Assessment of B. amyloliquefaciens (Ref. 6). Given that the natural
habitat for B. amyloliquefaciens is typically in soil, on plant roots,
or as an endophyte within the roots or stems of plants, the bacterium
is likely to survive for a least some period of time if inadvertently
released to the environment. However, like other bacilli, survival in
soil may occur predominately as the resistant endospore state, whereas
in the rhizosphere, it may exist as active vegetative cells.
VI. Physical Containment and Control Technologies for T. reesei QM6a
and B. amyloliquefaciens subsp. amyloliquefaciens
A. Release and Exposure Assessment in Support of the TSCA Section
5(h)(4) Exemption for T. reesei QM6a
The estimated releases of the microorganism from an enzyme
manufacturing facility and exposures of workers, the general
population, and the environment to the microorganisms are based on a
generic scenario developed by EPA in 1997 for large-scale closed system
enzyme fermentation. The generic scenario assumes the facility operates
350 days/year, produces 100 batches/year, the maximal cell
concentration in the fermentation broth is 1 x 10\7\ colony-forming
units (cfu)/ml, and the volume of the fermentation broth is 70,000 L.
The process consists of the main steps of laboratory propagation,
fermentation, inactivation, and recovery where filtration operations
separate out the microbial biomass from the concentrated desired
product. The operations, sources of exposure and release are described
in more detail in EPA's Release and Exposure Assessment (Ref. 13).
Exposures of workers to the microorganisms in during processing
operations using submerged standard industrial fermentation do not pose
concerns. The release of microbial cells in aerosols or in liquid and
solid waste streams in submerged standard industrial fermentation
operations with the containment and inactivation conditions of the Tier
I exemption, are considered low. Thus, potential exposures to the
general human population to the microorganism through inhalation or
drinking water ingestion and to the environment are also low.
[[Page 13768]]
B. Release and Exposure Assessment in Support of the TSCA Section
5(h)(4) Exemption for B. amyloliquefaciens subsp. amyloliquefaciens
The estimated releases of the microorganism from an enzyme
manufacturing facility and exposures of the microorganisms to workers,
the general population, and the environment are based on a generic
scenario developed by EPA in 1997 for large-scale closed system enzyme
fermentation. The generic scenario assumes the facility operates 350
days/year, produces 100 batches/year, the maximal cell concentration in
the fermentation broth is 1 x 10\11\ cfu/ml and the volume of the
fermentation broth is 70,000 L. The process consists of the main steps
of laboratory propagation, fermentation and then recovery where
filtration operations separate out the biomass from the concentrated
desired product. The operations, sources of exposure and release are
described in more detail in EPA's Release and Exposure Assessment (Ref.
14).
Exposures of workers to the microorganisms during processing
operations using submerged standard industrial fermentation do not pose
concerns. The release of microbial cells in aerosols or in liquid and
solid waste streams in submerged standard industrial fermentaion
operations with the containment and inactivation conditions of the Tier
I exemption are considered low. Thus, potential exposures to the
general human population to the microorganism through inhalation or
drinking water ingestion and to the environment are also low.
VII. Risk Assessment Overview for T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens
EPA's Risk Assessment documents (Refs. 5 and 6) provide more
detailed information, and supporting references, for EPA's evaluation
of the available information and the potential risks to health and the
environment. EPA has determined that because of the low hazard
potential and safe history of use of T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens, the TSCA section 5(h)(4)
exemption will not present an unreasonable risk of injury to health or
the environment, including an unreasonable risk of injury to a
potentially exposed or susceptible subpopulation under the conditions
of use, provided that the other conditions of the exemptions at 40 CFR
part 725, subpart G, relating to the introduced genetic material, and
the physical containment of the new microorganisms, have been met.
A. Risk Assessment for T. reesei QM6a
There is only one potential concern for human health and
environmental hazards associated with T. reesei QM6a, and that is for
paracelsin production. Paracelsin production is not expected to occur
in submerged standard industrial fermentation operations conducted
solely for growth of the microorganism to produce enzymes. There is no
concern for potential pathogenicity of T. reesei QM6a to humans,
plants, domesticated animals, or wildlife. The body of evidence of
pathogenicity testing on various industrial strains indicates that T.
reesei is not pathogenic to humans. Toxicity testing on a number of
enzymes produced by T. reesei indicates that the fungus does not
produce toxins when used in the submerged standard industrial
fermentation operations used for enzyme production.
T. reesei has a long history of safe use and is expected to present
low hazard to workers, the general public, and the environment.
Although direct monitoring data are unavailable, estimates of potential
exposures made by EPA in its assessment of potential risks (Ref. 5) do
not indicate high levels of exposure of T. reesei to either workers or
the public from submerged standard industrial fermentation operations
used for enzyme production. Standard industrial hygiene management
practices currently used in the fermentation industry reduce the
potential for adverse health effects in the workplace. The use of
engineering controls (closed fermentation systems), appropriate work
practices, personal protective equipment, and personal hygiene reduce
the potential for worker exposure. Thus, current practices reduce the
potential for the dermal and respiratory exposures estimated by EPA.
Based on worst-case exposure scenarios and toxicity of the
microorganism, EPA has made the determination that the potential risk
to workers, the general public, and to the environment resulting from
the use of T. reesei QM6a in submerged standard industrial fermentation
operations used for enzyme production is low, provided the additional
criteria of the tiered exemptions for the introduced genetic material
and the physical containment conditions are met (Ref. 5).
B. Risk Assessment for B. amyloliquefaciens subsp. amyloliquefaciens
Industrial strains of B. amyloliquefaciens subsp. amyloliquefaciens
are not pathogenic to humans, plants, domesticated animals, or
wildlife, and do not produce many of the toxic secondary metabolites
found in biological control strains of B. amyloliquefaciens subsp.
plantarum. The long history of safe use of enzymes produced by
industrial strains of B. amyloliquefaciens in food is evidence that the
bacterium does not produce toxins under standard conditions used for
enzyme production.
Current practices in the fermentation industry reduce the potential
for adverse health effects in the workplace. The use of engineering
controls (closed fermentation systems), appropriate work practices,
personal protective equipment, and personal hygiene reduce the
potential for worker exposure and reduce the potential for the dermal
and respiratory exposures.
Industrial strains of B. amyloliquefaciens have a long history of
safe use and are expected to present low hazard to workers, the general
public, and the environment. Although direct monitoring data are
unavailable, exposure estimates do not suggest high levels of exposure
of B. amyloliquefaciens subsp. amyloliquefaciens to either workers or
the public resulting from the industrial fermentation procedures that
are standard throughout the industry.
Based on worst-case exposure scenarios and toxicity of the
microorganism, EPA has made the determination that the potential risk
to workers, the general public, and the environment associated with the
use of industrial strains of B. amyloliquefaciens subsp.
amyloliquefaciens in submerged standard industrial fermentation is low
provided the additional criteria of the tiered exemptions for the
introduced genetic material and the physical containment conditions are
met (Ref. 6).
VIII. Rationale for Adding T. reesei QM6a and B. amyloliquefaciens
subsp. amyloliquefaciens to the List of Recipient Microorganisms at 40
CFR 725.420
A. Statutory Background
On June 22, 2016, the ``Frank R. Lautenberg Chemical Safety for the
21st Century Act,'' amended TSCA (15 U.S.C. 2601 et seq.) (Ref. 15).
Pursuant to TSCA section 5(h)(4), EPA is authorized, upon request and
by rule, to exempt the manufacturer of any new
[[Page 13769]]
chemical substance from all or part of the requirements of TSCA section
5 if EPA determines that the manufacture, processing, distribution in
commerce, use, or disposal of the chemical substance, or any
combination of such activities, will not present an unreasonable risk
of injury to human health or the environment, including an unreasonable
risk to a potentially exposed or susceptible subpopulation identified
by the Administrator under the conditions of use. The amended language
of the statute with regard to section 5(h)(4) did not alter EPA's
approach to balancing the considerations of the costs and benefits of
issuing an exemption rule.
B. EPA's Approach for Assessing ``Unreasonable Risk'' for T. reesei
QM6a and B. amyloliquefaciens subsp. amyloliquefaciens
In determining whether T. reesei QM6a and B. amyloliquefaciens
subsp. amyloliquefaciens will not present an unreasonable risk of
injury to human health or the environment, the Agency considered more
than just the inherent risks presented by the two microorganisms. The
Agency also considered the full range of societal benefits associated
with the exemption; for example, as discussed in more detail below, EPA
considered not only the cost savings to the users of the microorganism,
but also the societal benefits that flow from promotion of the use of
low-risk recipient microorganisms, while allowing the Agency to direct
its resources toward reviewing higher risk microorganisms.
It is important that EPA is revising one aspect of the existing
tiered exemptions at 40 CFR 725.420 by expanding the exemption to apply
to two specific microorganisms. The narrow scope of this action
affected the scope of EPA's cost-benefit analysis in which EPA compared
the risks and benefits of the two microorganisms being considered for
an exemption with the risks that would have resulted if those same two
microorganisms remained subject to full MCAN submission requirements
and 90-day EPA review. EPA did not compare the risks and benefits that
would result from use of these two microorganisms in the absence of any
regulation.
It is also significant that the standard applicable to this rule is
that the microorganisms ``will not present unreasonable risk,'' rather
than ``no risk.'' It is not possible to eliminate all risks associated
with the manufacture, processing, distribution in commerce, use, and
disposal of any new microorganism.
C. Application of No Unreasonable Risk Factors for T. reesei QM6a and
B. amyloliquefaciens subsp. amyloliquefaciens
The following is an explanation of the factors and their analyses
relevant to the no unreasonable risk finding.
1. Risks associated with these two microorganisms. EPA's evaluation
of the available information concerning T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens against these criteria is
presented in detail in Unit V., and is summarized again here for the
readers' convenience.
The Agency developed specific criteria in 40 CFR 725.67 that the
Agency uses in determining the extent of a potential recipient
microorganism's risks, and its eligibility for listing at 40 CFR
725.420. These criteria were explained in detail in the proposed
``biotech'' rule (Ref. 16), the final ``biotech'' rule (Ref. 17), and
are discussed in Unit V. EPA's conclusions for these two microorganisms
are based on the available data and EPA's experience under 40 CFR part
725. T. reesei QM6a is not pathogenic to humans, plants, domesticated
animals, or wildlife and the fungus does not produce toxins under
submerged standard industrial fermentation operations used for enzyme
production. T. reesei QM6a has a long history of safe use and is
generally expected to present low risk to workers, the general public,
and the environment resulting from submerged standard industrial
fermentation operations used for enzyme production that are standard
throughout the industry.
Under non-standard conditions of fermentation, such as with the
deliberate fermentation of cellulosic biomass for saccharification of
plant material or extended fermentation, paracelsin may be produced.
The risks associated with the production of paracelsin may be
significant due to its toxicity to mammalian cells, aquatic species,
Gram-positive bacteria, and various fungi. However, the potential risk
associated with paracelsin production is expected to be significantly
reduced by this rule, which limits the exemption to fermentation
operations using submerged standard industrial fermentation operations
used for enzyme production.
Industrial strains of B. amyloliquefaciens subspecies
amyloliquefaciens are not pathogenic to humans, plants, domesticated
animals, or wildlife, and do not produce toxins under standard
conditions used for enzyme production. Industrial strains of B.
amyloliquefaciens subsp. amyloliquefaciens used for the production of
enzymes have a long history of safe use and are expected to present low
hazards to human health and the environment.
Only strains of B. amyloliquefaciens that fall into the subspecies
B. amyloliquefaciens amyloliquefaciens were considered as the eligible
recipient microorganism at 40 CFR 725.420. In this rule, EPA is
excluding other strains/subspecies of these two species for which:
The Agency has insufficient data and review experience to
find that they will not present an unreasonable risk of injury or
The Agency has found that, under certain conditions, based
on data on the species in question, a strain or subspecies may present
an unreasonable risk, thereby requiring a closer examination of the
conditions of manufacturing, processing, distribution in commerce, use,
and disposal during a 90-day MCAN review. Consequently, additional
information would be necessary to make an appropriate determination
about the organisms' potential risks.
The Agency believes that the requirement for submission of a MCAN
followed by a 90-day review period for new intergeneric microorganisms
that use T. reesei QM6a and B. amyloliquefaciens subsp.
amyloliquefaciens as recipient microorganisms is not necessary to
address the risks associated with these microorganisms and would not
result in any additional protection than would be achieved by this
rule. This conclusion is based, in part, on EPA's findings regarding
the intrinsically low level of hazard that these two organisms pose to
human health and the environment. The requirements of the Tier I and
Tier II exemptions and the restrictions in this rule on fermentation
conditions place sufficient constraints to significantly limit the
potential risks of injury to human health or the environment, including
potential risks to potentially exposed or susceptible subpopulations
under the conditions of use. In making this determination, EPA
identified workers as a potentially exposed or susceptible
subpopulation to the substance under the conditions of use and
concluded that, with the limitations described above, the substances
will not present an unreasonable risk of injury to health or the
environment.
The Agency concludes that the criteria set forth in this rule are
sufficient to mitigate the identified risks associated with these
microorganisms. Because of the low hazard potential and safe history of
use of T. reesei QM6a and
[[Page 13770]]
B. amyloliquefaciens subsp. amyloliquefaciens, EPA concludes that the
TSCA section 5(h)(4) exemption will not present an unreasonable risk of
injury to health or the environment, including an unreasonable risk of
injury to a potentially exposed or susceptible subpopulation under the
conditions of use, provided that the other conditions of the exemptions
at 40 CFR part 725, subpart G, relating to the introduced genetic
material, and the physical containment of the new microorganisms, have
been met.
2. Costs. As discussed in Unit X., this rule is anticipated to
reduce costs to currently regulated entities in the long run. Expanding
the list of recipient microorganisms eligible for exemption does not
otherwise impose any additional cost or other burden on currently
regulated entities, or existing fermentation processes.
Limiting the use of this exemption to the identified fermentation
conditions is also estimated to impose no burden on affected entities.
The restriction merely codifies existing industrial fermentation
procedures for manufacturing operations that currently seek to use
tiered exemptions. Consequently, EPA expects that most, if not all,
manufacturers using these microbes would already have the measures in
place to qualify for the exemption. Equally important, this limitation
would add no burden to any existing fermentation processes. Currently,
fermentation operations with either of these microbes are not eligible
for the tiered exemption, and thus a MCAN must be submitted. Any
company that chooses to use a different fermentation process could
continue to operate under the status quo and simply submit a MCAN. This
rule simply offers an additional, less costly option, to facilities
that choose to use the fermentation operations discussed in this rule.
3. Benefits. The following discussion describes the benefits of
expanding the list of recipient microorganisms eligible for exemption
in a qualitative manner; for a more quantitative approach, see the
economic analysis prepared for this rule (Ref. 18). A summary of that
economic analysis is also provided in Unit IX.
The benefits analyzed encompass more than the direct benefits
associated with submitting a Tier I or Tier II exemption for a new
intergeneric microorganism rather than a MCAN. EPA's benefit analysis
included a consideration of the broader benefits to society. EPA's
unreasonable risk determination is based on broader benefits to society
as well as those benefits attributable to a reduction in the burden
associated with submission of Tier I and Tier II exemptions rather than
MCANs.
EPA has concluded that manufacturers of new intergeneric
microorganisms based on these low-risk microorganisms currently bear an
unnecessary regulatory burden. By adding T. reesei QM6a and B.
amyloliquefaciens subsp. amyloliquefaciens to the list of eligible
recipient microorganisms in 40 CFR 725.420, the Agency removes
unnecessary regulatory impediments to the design, manufacture, and
commercialization of these low risk new intergeneric microorganisms,
and of the chemical substances that can be produced by these safer
microorganisms. This action will also reduce the costs associated with
industry's reporting burden, including the costs associated with the
preparation of the submission, and with the delay in the commercial
market introduction of the new intergeneric microorganism. Some of the
cost-savings benefits may accrue to small businesses, either as
developers of the exempt microorganisms, as producers of fermentation
chemicals using the live microorganisms, or as customers for enzymes or
other products made using the microorganisms.
There will also be a reduction in the Agency review resources
currently allocated to reviews of MCANs for these two microorganisms.
These Agency resources will be shifted to the review of new
intergeneric microorganisms or chemical substances of greater concern.
The addition of the two microorganisms to the list of
microorganisms eligible for exemption is expected to encourage
innovation in the industry. It is reasonable to assume that a new
intergeneric microorganism would either possess a new function or serve
an existing function more efficiently or at a lower cost. The reduction
in delay for that new intergeneric microorganism to be introduced into
commerce is expected to be a benefit to both manufacturers and the
general public who will have access to the substance more quickly. The
expected benefits to innovation have not been quantified but include:
Reduced time to develop and commercialize organisms; decreased cost of
some downstream industrial products, such as fuel ethanol; improved
consumer appeal of some products, such as certain textiles; and reduced
costs of some consumer products, such as detergent and leather goods.
4. Risk/benefit balance. Determining the presence or absence of an
unreasonable risk for purposes of issuing an exemption pursuant to TSCA
section 5(h)(4) requires balancing of the benefits and risks posed by a
regulatory action. EPA has determined that the risks are generally low
based on the inherent properties and intended uses of T. reesei QM6a
and B. amyloliquefaciens subsp. amyloliquefaciens and will be
adequately managed by the restrictions in the rule, combined with the
existing requirements of the Tier I and Tier II exemptions.
EPA anticipates that expanding the list of microorganisms eligible
for exemption will impose no costs and will reduce costs to currently
regulated entities that use those recipients. The limitation to certain
fermentation conditions is not a cost that will be imposed by this rule
but rather a limitation on the amount of regulatory relief it will
provide. The limitations on fermentation conditions reflect industrial
fermentation procedures that are currently common practices for the
affected industry.
EPA has also concluded that the benefits of the addition of T.
reesei QM6a and B. amyloliquefaciens subsp. amyloliquefaciens as
recipient microorganisms to the list of recipient microorganisms at 40
CFR 725.420 are quite significant. This addition reduces the overall
regulatory burden for affected entities by reducing the reporting
requirements and by eliminating the delay of these products into
commerce. The rule benefits both regulated entities and the general
public by promoting the expedited manufacture and use of the chemical
substances produced using these low-risk organisms and manufacturing
processes. There is also the added benefit of concentrating limited EPA
resources on regulation of chemical substances which have a greater
potential to present significant risks, rather than on these two
microorganisms. While this is difficult to quantify, it is considered
substantial.
In sum, the criteria set forth in this exemption are sufficient to
mitigate the low level of potential risks presented by these organisms,
particularly when compared to the benefits, in toto, of this exemption,
to levels that are consistent with the statutory standard for an
exemption. Consequently, EPA has determined that adding T. reesei QM6a
and B. amyloliquefaciens subsp. amyloliquefaciens as recipient
microorganisms to the list of recipient microorganisms at 40 CFR
725.420 is appropriate. The two microorganisms
[[Page 13771]]
will not present an unreasonable risk of injury to human health or the
environment when manufactured under the conditions of this exemption.
IX. Economic Impacts
EPA's economic analysis (Ref. 18) evaluates the potential for
significant economic impacts as a result of the addition of two
microorganisms (T. reesei QM6a and B. amyloliquefaciens subsp.
amyloliquefaciens) to 40 CFR 725.420, which lists recipient
microorganisms eligible for Tier I and Tier II exemptions. Over the
course of the first 10 years after the effective date of the final
rule, EPA estimates that the addition of the two microorganisms to the
list will generate a total cost savings to society of approximately
$4.5 million. Industry is estimated save approximately $2.7 million and
the Agency approximately $1.8 million. The equivalent, annualized cost
savings to industry are expected to be $260,000 per year and $252,000
per year at a 3% and 7% discount rate, respectively. EPA estimates that
there will be a net decrease in burden to industry of 27,864 hours over
this 10-year period.
X. Scientific Standards, Evidence, and Available Information
EPA has used scientific information, technical procedures,
measures, methods, protocols, methodologies, and models consistent with
the best available science, as applicable. These sources supply
information relevant to a determination that the microorganisms subject
to this rule will not present an unreasonable risk of injury to health
or the environment, including an unreasonable risk to a potentially
exposed or susceptible subpopulation identified by the Administrator
under the conditions of use. The clarity and completeness of the data,
assumptions, methods, quality assurance, and analyses employed are
documented, as applicable and to the extent necessary for purposes of
this rule, in Units V. through VIII. and in the references. The extent
to which the various information, procedures, measures, methods,
protocols, methodologies or models used in EPA's decision have been
subject to independent verification or peer review is adequate to
justify their use, collectively, in the record for this rule.
XI. References
The following is a listing of the documents that are specifically
referenced in this document. The docket includes these documents and
other information considered by EPA, including documents that are
referenced within the documents that are in the docket, even if the
referenced document is not physically located in the docket. For
assistance in locating these other documents, please consult the
technical person listed under FOR FURTHER INFORMATION CONTACT.
1. Genencor International, Inc. Letter of Application to list
Trichoderma reesei as exempt under subpart G of 40 CFR part 725--
Reporting Requirements and Review Processes for Microorganisms.
March 17, 2005.
2. Novo Nordisk BioChem North America, Inc. Letter of
Application to list Bacillus amyloliquefaciens as exempt under
subpart G of 40 CFR part 725--Reporting Requirements and Review
Processes for Microorganisms. November 7, 1997.
3. EPA, OPPT. Email confirming Novo Nordisk BioChem North
America, Inc.'s letter of application to list Bacillus
amyloliquefaciens as exempt under subpart G of 40 CFR part 725--
Reporting Requirements and Review Processes for Microorganisms.
August 3, 2009.
4. US EPA. Microorganisms; General Exemptions from Reporting
Requirements; Revisions to Recipient Organisms Eligible for Tier I
and Tier II Exemptions; Proposed Rule. RIN 2070-AJ65; FRL-9348-1. 77
FR 54499, September 5, 2012. (``2012 Proposed Rule'').
5. EPA, OPPT. Risk Assessment of Trichoderma reesei for
Consideration of Addition to the List of Eligible Recipient
Microorganisms for the 5(h)(4) Exemptions from MCAN Reporting
Requirements. October 2011.
6. EPA, OPPT. Risk Assessment of Bacillus amyloliquefaciens
subsp. amyloliquefaciens for Consideration of Addition to the List
of Eligible Recipient Microorganisms for the 5(h)(4) Exemptions from
MCAN Reporting Requirements. July 2015.
7. Anonymous Public Comment, Document ID: EPA-HQ-OPPT-2011-0740-
0015; October 23, 2012.
8. Richard Fitti, West Chester University of PA Comment,
Document ID: EPA-HQ-OPPT-2011-0740-0017; November 5, 2012.
9. Anthony T. Pavel, General Counsel & Secretary, Enzyme
Technical Association (ETA) and Rina Singh, Director of Policy,
Science & Renewable Chemicals, Industrial and Environmental Section,
Biotechnology Industry Organization (BIO) Comment, Document ID EPA-
HQ-OPPT-2011-0740-0016; November 2012.
10. ETA. Supplemental information on Trichoderma reesei. January
29, 2010.
11. ETA. Supplemental information on Trichoderma reesei. June
16, 2011.
12. Nevalainen, H., P. Suominen, K. Tasimisto. 1994. On the
safety of Trichoderma reesei. J. Biotechol. 37:193-200.
13. EPA, OPPT. Release and Exposure Assessment in Support of the
TSCA Section 5(h)(4) Exemption for Trichoderma reesei. June 2011.
14. EPA, OPPT. Release and Exposure Assessment in Support of the
TSCA Section 5(h)(4) Exemption for Bacillus amyloliquefaciens. June
2011.
15. Legislative History of the Toxic Substances Control Act, pp.
409-423. House Report 1341, 94th Congress, 2nd Session. 1976.
16. EPA. Microbial Products of Biotechnology; Proposed
Regulation under the Toxic Substances Control Act. Federal Register
(59 FR 45526; September 1, 1994) (FRL-4774-4).
17. EPA. Microbial Products of Biotechnology; Final Regulation
under the Toxic Substances Control Act. Federal Register (62 FR
17910; April 11, 1997) (FRL-5577-2).
18. EPA, OPPT. Economic Analysis for the Final Biotechnology
Exemptions Rule for Trichoderma reesei and Bacillus
amyloliquefaciens. October 2019.
XII. Statutory and Executive Order Reviews
Additional information about these statutes and Executive Orders
can be found at https://www2.epa.gov/laws-regulations/laws-and-executive-orders.
A. Executive Order 12866: Regulatory Planning and Review and Executive
Order 13563: Improving Regulations and Regulatory Review
This action is not a significant regulatory action and was
therefore not submitted to the Office of Management and Budget (OMB)
for review under Executive Orders 12866 (58 FR 51735, October 4, 1993)
and 13563 (76 FR 3821, January 21, 2011).
B. Executive Order 13771: Reducing Regulations and Controlling
Regulatory Costs
This is considered a deregulatory action under Executive Order
13771 (82 FR 9339, February 3, 2017) because this rule is expected to
provide meaningful burden reduction by adding T. reesei and B.
amyloliquefaciens subspecies amyloliquefaciens to the list of recipient
microorganisms that may be used to qualify for the Tier I and Tier II
exemptions from full notification and reporting under TSCA for new
microorganisms that are being manufactured for introduction into
commerce. The rule is expected to generate cost savings for
organizations that, in the absence of the rule, would submit MCANs for
new intergeneric T. reesei or B. amyloliquefaciens strains. EPA
estimates that the rule will result in cost savings for both industry
and the Agency.
C. Paperwork Reduction Act (PRA)
This action does not impose any new information collection
requirements or related burden that would require additional review or
approval by OMB under the PRA, 44 U.S.C. 3501 et seq. The information
collection activities associated with the submission of Tier 1 and Tier
2 notices under TSCA have already been approved by OMB
[[Page 13772]]
pursuant to the PRA and are covered by the following existing
Information Collection Requests (ICRs): OMB control numbers 2070-0012
(EPA ICR No. 0574.15) and 2070-0038 (EPA ICR No. 1188.11). In granting
these exemptions, this rule does not impose any new information
collection requirements and is expected to reduce the amount of
required reporting by allowing firms to submit less information for
qualifying microorganisms. Over the ten-year period, industry is
expected to subtract a total of 27,864 hours at an average of 2,786
hours per year.
D. Regulatory Flexibility Act (RFA)
Pursuant to section 605(b) of the RFA, 5 U.S.C. 601 et seq., I
certify that this final rule will not have a significant economic
impact on a substantial number of small entities. In making this
determination, EPA believes that the impact of concern is any adverse
economic impact on small entities, and that EPA may certify that a rule
will not have a significant economic impact on a substantial number of
small entities if the rule relieves regulatory burden, has no net
burden or otherwise has a positive economic effect on the small
entities subject to the rule. This action establishes exemptions from
existing requirements that apply regardless of the size of the entity.
The factual basis for this certification is presented in the small
entity impact analysis that was prepared as part of the Economic
Analysis for this rule (Ref. 18) and is briefly summarized in Unit
VIII.
E. Unfunded Mandates Reform Act (UMRA)
This action does not contain an unfunded mandate as described in
UMRA, 2 U.S.C. 1531-1538, and does not significantly or uniquely affect
small governments. This action is not expected to impose enforceable
duty on any state, local or tribal governments, and the requirements
imposed on the private sector are not expected to result in annual
expenditures of $100 million or more for the private sector. As such,
EPA has determined that the requirements of UMRA sections 202, 203,
204, or 205 do not apply to this action.
F. Executive Order 13132: Federalism
This action does not have federalism implications as specified in
Executive Order 13132 (64 FR 43255, August 10, 1999). It will not have
substantial direct effects on the states, on the relationship between
the national government and the states, or on the distribution of power
and responsibilities among the various levels of government. EPA has no
information to indicate that any state or local government commercially
manufactures or processes the microorganisms covered by this action.
Thus, Executive Order 13132 does not apply to this action.
G. Executive Order 13175: Consultation and Coordination With Indian
Tribal Governments
This action does not have tribal implications as specified in
Executive Order 13175 (65 FR 67249, November 9, 2000). It will not have
substantial direct effects on tribal governments, on the relationship
between the Federal government and the Indian tribes, or on the
distribution of power and responsibilities between the Federal
government and Indian tribes. EPA has no information to indicate that
any tribal government commercially manufactures or processes the
microorganisms covered by this action. Thus, E.O. 13175 does not apply
to this action.
H. Executive Order 13045: Protection of Children From Environmental
Health Risks and Safety Risks
EPA interprets Executive Order 13045 (62 FR 19885, April 23, 1997),
as applying only to those regulatory actions that concern health or
safety risks, such that the analysis required under section 5-501 of
Executive Order 13045 has the potential to influence the regulation.
This action is not subject to Executive Order 13045 because it does not
establish an environmental standard intended to mitigate health or
safety risks.
I. Executive Order 13211: Actions That Significantly Affect Energy
Supply, Distribution, or Use
This action is not a ``significant energy action'' as defined in
Executive Order 13211 (66 FR 28355, May 22, 2001), because it is not a
significant regulatory action under Executive Order 12866, and is not
likely to have a significant adverse effect on energy supply,
distribution, or use.
J. National Technology Transfer and Advancement Act (NTTAA)
Since this action does not involve any technical standards, NTTAA
section 12(d), 15 U.S.C. 272 note, does not apply to this action.
K. Executive Order 12898: Federal Actions to Address Environmental
Justice in Minority Populations and Low-income Populations
This action does not entail special considerations of environmental
justice related issues as delineated by Executive Order 12898 (59 FR
7629, February 16, 1994), because it does not establish an
environmental health or safety standard.
VII. Congressional Review Act (CRA)
This action is subject to the CRA, 5 U.S.C. 801 et seq., and EPA
will submit a rule report to each House of the Congress and to the
Comptroller General of the United States. This action is not a ``major
rule'' as defined by 5 U.S.C. 804(2).
List of Subjects in 40 CFR Part 725
Environmental protection, Administrative practice and procedure,
Biotechnology, Chemicals, Hazardous substances, Imports, Labeling,
Microorganisms, Occupational safety and health, Reporting and
recordkeeping requirements.
Dated: March 4, 2020.
Alexandra Dapolito Dunn,
Assistant Administrator, Office of Chemical Safety and Pollution
Prevention.
Therefore, 40 CFR chapter I is amended as follows:
PART 725--[AMENDED]
0
1. The authority citation for part 725 continues to read as follows:
Authority: 15 U.S.C. 2604, 2607, 2613, and 2625.
0
2. In Sec. 725.3, add in alphabetical order a definition for
``Submerged standard industrial fermentation'' to read as follows:
Sec. 725.3 Definitions.
* * * * *
Submerged standard industrial fermentation means a fermentation
system that meets all of the following conditions:
(1) Enzyme production is conducted under conditions of submerged
fermentation (i.e., growth of the microorganism occurs beneath the
surface of the liquid growth medium).
(2) Any fermentation of solid plant material or insoluble
substrates, to which T. reesei fermentation broth is added after the
submerged standard industrial fermentation operations used for enzyme
production is completed, may be initiated only after the inactivation
of the microorganism as delineated in 40 CFR 725.422(d).
* * * * *
0
3. In Sec. 725.420, add paragraphs (k) and (l) to read as follows:
Sec. 725.420 Recipient microorganisms.
* * * * *
(k) Trichoderma reesei strain QM6a and its derivatives used only in
[[Page 13773]]
submerged standard industrial fermentation operations as defined at 40
CFR 725.3.
(l) Bacillus amyloliquefaciens subsp. amyloliquefaciens.
[FR Doc. 2020-04746 Filed 3-9-20; 8:45 am]
BILLING CODE 6560-50-P
