Medical Devices; Hematology and Pathology Devices; Classification of a Cervical Intraepithelial Neoplasia Test System, 232-234 [2017-28342]
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Federal Register / Vol. 83, No. 2 / Wednesday, January 3, 2018 / Rules and Regulations
instructions, and specifies that action as RC:
This AD requires using a method approved
in accordance with the procedures specified
in paragraph (j) of this AD.
(i) Credit for Previous Actions
This paragraph provides credit for the
actions specified in paragraph (g) of this AD,
if those actions were performed before the
effective date of this AD using Boeing Alert
Service Bulletin 757–53A0100, dated
November 14, 2016.
jstallworth on DSKBBY8HB2PROD with RULES
(j) Alternative Methods of Compliance
(AMOCs)
(1) The Manager, Los Angeles ACO Branch,
FAA, has the authority to approve AMOCs
for this AD, if requested using the procedures
found in 14 CFR 39.19. In accordance with
14 CFR 39.19, send your request to your
principal inspector or local Flight Standards
District Office, as appropriate. If sending
information directly to the manager of the
certification office, send it to the attention of
the person identified in paragraph (k)(1) of
this AD. Information may be emailed to 9ANM-LAACO-AMOC-Requests@faa.gov.
(2) Before using any approved AMOC,
notify your appropriate principal inspector,
or lacking a principal inspector, the manager
of the local flight standards district office/
certificate holding district office.
(3) An AMOC that provides an acceptable
level of safety may be used for any repair,
modification, or alteration required by this
AD if it is approved by the Boeing
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Designation Authorization (ODA) that has
been authorized by the Manager, Los Angeles
ACO Branch, to make those findings. To be
approved, the repair method, modification
deviation, or alteration deviation must meet
the certification basis of the airplane, and the
approval must specifically refer to this AD.
(4) Except as required by paragraph (h)(2)
of this AD: For service information that
contains steps that are labeled as RC, the
provisions of paragraphs (j)(4)(i) and (j)(4)(ii)
of this AD apply.
(i) The steps labeled as RC, including
substeps under an RC step and any figures
identified in an RC step, must be done to
comply with the AD. If a step or substep is
labeled ‘‘RC Exempt,’’ then the RC
requirement is removed from that step or
substep. An AMOC is required for any
deviations to RC steps, including substeps
and identified figures.
(ii) Steps not labeled as RC may be
deviated from using accepted methods in
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or inspection program without obtaining
approval of an AMOC, provided the RC steps,
including substeps and identified figures, can
still be done as specified, and the airplane
can be put back in an airworthy condition.
(k) Related Information
(1) For more information about this AD,
contact Muoi Vuong, Aerospace Engineer,
Airframe Section, FAA, Los Angeles ACO
Branch, 3960 Paramount Boulevard,
Lakewood, CA 90712–4137; phone: 562–627–
5205; fax: 562–627–5210; email:
muoi.vuong@faa.gov.
(2) Service information identified in this
AD that is not incorporated by reference is
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available at the addresses specified in
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part 51.
(2) You must use this service information
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this AD, unless the AD specifies otherwise.
(i) Boeing Alert Service Bulletin 757–
53A0100, Revision 1, dated September 14,
2017.
(ii) Reserved.
(3) For service information identified in
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Airplanes, Attention: Contractual & Data
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MC 110–SK57, Seal Beach, CA 90740;
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www.myboeingfleet.com.
(4) You may view this service information
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Issued in Renton, Washington, on
December 14, 2017.
Jeffrey E. Duven,
Director, System Oversight Division, Aircraft
Certification Service.
[FR Doc. 2017–28148 Filed 1–2–18; 8:45 am]
BILLING CODE 4910–13–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
21 CFR Part 864
[Docket No. FDA–2017–N–6599]
Medical Devices; Hematology and
Pathology Devices; Classification of a
Cervical Intraepithelial Neoplasia Test
System
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Final order.
The Food and Drug
Administration (FDA or we) is
classifying the cervical intraepithelial
neoplasia (CIN) test system into class II
(special controls). The special controls
that apply to the device type are
identified in this order and will be part
of the codified language for the CIN test
system’s classification. We are taking
this action because we have determined
SUMMARY:
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that classifying the device into class II
(special controls) will provide a
reasonable assurance of safety and
effectiveness of the device. We believe
this action will also enhance patients’
access to beneficial innovative devices,
in part by reducing regulatory burdens.
DATES: This order is effective January 3,
2018. The classification was applicable
on March 4, 2017.
FOR FURTHER INFORMATION CONTACT:
Steven Tjoe, Center for Devices and
Radiological Health, Food and Drug
Administration, 10903 New Hampshire
Ave., Bldg. 66, Rm. 4550, Silver Spring,
MD 20993–0002, 301–796–5866,
steven.tjoe@fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
I. Background
Upon request, FDA has classified the
cervical intraepithelial neoplasia (CIN)
test system as class II (special controls),
which we have determined will provide
a reasonable assurance of safety and
effectiveness. In addition, we believe
this action will enhance patients’ access
to beneficial innovation, in part by
reducing regulatory burdens by placing
the device into a lower device class than
the automatic class III assignment.
The automatic assignment of class III
occurs by operation of law and without
any action by FDA, regardless of the
level of risk posed by the new device.
Any device that was not in commercial
distribution before May 28, 1976, is
automatically classified as, and remains
within, class III and requires premarket
approval unless and until FDA takes an
action to classify or reclassify the device
(see 21 U.S.C. 360c(f)(1)). We refer to
these devices as ‘‘postamendments
devices’’ because they were not in
commercial distribution prior to the
date of enactment of the Medical Device
Amendments of 1976, which amended
the Federal Food, Drug, and Cosmetic
Act (FD&C Act).
FDA may take a variety of actions in
appropriate circumstances to classify or
reclassify a device into class I or II. We
may issue an order finding a new device
to be substantially equivalent under
section 513(i) of the FD&C Act (21
U.S.C. 360c(i)) to a predicate device that
does not require premarket approval.
We determine whether a new device is
substantially equivalent to a predicate
by means of the procedures for
premarket notification under section
510(k) of the FD&C Act and part 807 (21
U.S.C. 360(k) and 21 CFR part 807,
respectively).
FDA may also classify a device
through ‘‘De Novo’’ classification, a
common name for the process
authorized under section 513(f)(2) of the
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Federal Register / Vol. 83, No. 2 / Wednesday, January 3, 2018 / Rules and Regulations
FD&C Act. Section 207 of the Food and
Drug Administration Modernization Act
of 1997 established the first procedure
for De Novo classification (Pub. L. 105–
115). Section 607 of the Food and Drug
Administration Safety and Innovation
Act modified the De Novo application
process by adding a second procedure
(Pub. L. 112–144). A device sponsor
may utilize either procedure for De
Novo classification.
Under the first procedure, the person
submits a 510(k) for a device that has
not previously been classified. After
receiving an order from FDA classifying
the device into class III under section
513(f)(1) of the FD&C Act, the person
then requests a classification under
section 513(f)(2).
Under the second procedure, rather
than first submitting a 510(k) and then
a request for classification, if the person
determines that there is no legally
marketed device upon which to base a
determination of substantial
equivalence, that person requests a
classification under section 513(f)(2) of
the FD&C Act.
Under either procedure for De Novo
classification, FDA shall classify the
device by written order within 120 days.
The classification will be according to
the criteria under section 513(a)(1) of
the FD&C Act. Although the device was
automatically placed within class III,
the De Novo classification is considered
to be the initial classification of the
device.
We believe this De Novo classification
will enhance patients’ access to
beneficial innovation, in part by
reducing regulatory burdens. When FDA
classifies a device into class I or II via
the De Novo process, the device can
serve as a predicate for future devices of
that type, including for 510(k)s (see 21
U.S.C. 360c(f)(2)(B)(i)). As a result, other
device sponsors do not have to submit
a De Novo request or premarket
approval application in order to market
a substantially equivalent device (see 21
U.S.C. 360c(i), defining ‘‘substantial
equivalence’’). Instead, sponsors can use
the less-burdensome 510(k) process,
when necessary, to market their device.
II. De Novo Classification
On May 23, 2016, Ventana Medical
Systems, Inc., submitted a request for De
Novo classification of the CINtec
Histology. FDA reviewed the request in
order to classify the device under the
criteria for classification set forth in
section 513(a)(1) of the FD&C Act. We
classify devices into class II if general
controls by themselves are insufficient
to provide reasonable assurance of
safety and effectiveness, but there is
sufficient information to establish
special controls that, in combination
with the general controls, provide
reasonable assurance of the safety and
effectiveness of the device for its
intended use (see 21 U.S.C.
360c(a)(1)(B)). After review of the
information submitted in the request,
we determined that the device can be
classified into class II with the
establishment of special controls. FDA
has determined that these special
controls, in addition to the general
controls, will provide reasonable
assurance of the safety and effectiveness
of the device.
Therefore, on March 4, 2017, FDA
issued an order to the requestor
classifying the device into class II. FDA
is codifying the classification of the
device by adding 21 CFR 864.1865. We
have named the generic type of device
the cervical intraepithelial neoplasia
(CIN) test system, and it is identified as
a device used to detect a biomarker
associated with CIN in human tissues.
The device is indicated as an adjunct
test and not to be used as a stand-alone
device. The test results must be
interpreted in the context of the
patient’s clinical history including, but
not limited to, prior and current cervical
biopsy results, Papanicolaou (Pap) test
results, human papillomavirus (HPV)
test results, and morphology on
hematoxylin and eosin (H&E) stained
sections. This device is not intended to
detect the presence of HPV.
FDA has identified the following risks
to health associated specifically with
this type of device and the measures
required to mitigate these risks in table
1.
TABLE 1—CERVICAL INTRAEPITHELIAL NEOPLASIA (CIN) TEST SYSTEM RISKS TO HEALTH AND REQUIRED MITIGATIONS
Identified risks
Required mitigations/21 CFR section
Inaccurate test results, such as false positive or false negative results
jstallworth on DSKBBY8HB2PROD with RULES
Failure to correctly interpret test results can lead to false positive or
false negative results.
FDA has determined that special
controls, in combination with the
general controls, address these risks to
health and provide reasonable assurance
of safety and effectiveness. For a device
to fall within this classification, and
thus avoid automatic classification in
class III, it would have to comply with
the special controls named in this final
order. The necessary special controls
appear in the regulation codified by this
order. This device is subject to
premarket notification requirements
under section 510(k) of the FD&C Act.
III. Analysis of Environmental Impact
The Agency has determined under 21
CFR 25.34(b) that this action is of a type
that does not individually or
cumulatively have a significant effect on
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General controls and special controls
864.1865(b)(1); 21 CFR 864.1865(b)(2)).
General controls and special controls
864.1865(b)(1); 21 CFR 864.1865(b)(2)).
the human environment. Therefore,
neither an environmental assessment
nor an environmental impact statement
is required.
IV. Paperwork Reduction Act of 1995
This final order establishes special
controls that refer to previously
approved collections of information
found in other FDA regulations. These
collections of information are subject to
review by the Office of Management and
Budget (OMB) under the Paperwork
Reduction Act of 1995 (44 U.S.C. 3501–
3520). The collections of information in
21 CFR parts 801 and 809, regarding
labeling, have been approved under
OMB control number 0910–0485; the
collections of information in part 807,
subpart E, regarding premarket
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(1)
and
(2)
(21
CFR
(1)
and
(2)
(21
CFR
notification submissions, have been
approved under OMB control number
0910–0120; the collections of
information in 21 CFR part 814,
subparts A through E, regarding
premarket approval, have been
approved under OMB control number
0910–0231; and the collections of
information in the guidance document
‘‘De Novo Classification Process
(Evaluation of Automatic Class III
Designation)’’ have been approved
under OMB control number 0910–0844.
List of Subjects in 21 CFR Part 864
Blood, Medical devices, Packaging
and containers.
Therefore, under the Federal Food,
Drug, and Cosmetic Act and under
authority delegated to the Commissioner
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Federal Register / Vol. 83, No. 2 / Wednesday, January 3, 2018 / Rules and Regulations
of Food and Drugs, 21 CFR part 864 is
amended as follows:
PART 864—HEMATOLOGY AND
PATHOLOGY DEVICES
1. The authority citation for part 864
continues to read as follows:
■
Authority: 21 U.S.C. 351, 360, 360c, 360e,
360j, 360l, 371.
2. Add § 864.1865 to subpart B to read
as follows:
■
jstallworth on DSKBBY8HB2PROD with RULES
§ 864.1865 Cervical intraepithelial
neoplasia (CIN) test system.
(a) Identification. A cervical
intraepithelial neoplasia (CIN) test
system is a device used to detect a
biomarker associated with CIN in
human tissues. The device is indicated
as an adjunct test and not to be used as
a stand-alone device. The test results
must be interpreted in the context of the
patient’s clinical history including, but
not limited to, prior and current cervical
biopsy results, Papanicolaou (Pap) test
results, human papillomavirus (HPV)
test results, and morphology on
hematoxylin and eosin (H&E) stained
sections. This device is not intended to
detect the presence of HPV.
(b) Classification. Class II (special
controls). The special controls for this
device are:
(1) Premarket notification
submissions must include the following
information:
(i) The indications for use must
specify the biomarker that is intended to
be identified and its adjunct use (e.g.,
adjunct to examination of H&E stained
slides) to improve consistency in the
diagnosis of CIN.
(ii) Summary of professional society
recommendations, as applicable.
(iii) A detailed device description
including:
(A) A detailed description of all test
components, including all provided
reagents and required, but not provided,
ancillary reagents.
(B) A detailed description of
instrumentation and equipment,
including illustrations or photographs of
non-standard equipment or manuals.
(C) If applicable, detailed
documentation of the device software,
including, but not limited to, standalone software applications and
hardware-based devices that incorporate
software.
(D) A detailed description of
appropriate positive and negative
controls that are recommended or
provided.
(E) Detailed specifications for sample
collection, processing, and storage.
(F) A detailed description of
methodology and assay procedure.
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(G) A description of the assay cutoff
(the medical decision point between
positive and negative) or other relevant
criteria that distinguishes positive and
negative results, including the rationale
for the chosen cutoff or other relevant
criteria and results supporting
validation of the cutoff.
(H) Detailed specification of the
criteria for test results interpretation and
reporting.
(iv) Detailed information
demonstrating the performance
characteristics of the device, including:
(A) Analytical specificity studies such
as, but not limited to, antibody
characterization (e.g., Western Blot,
peptide inhibition analysis), studies
conducted on panels of normal tissues
and neoplastic tissues, interference by
endogenous and exogenous substances
as well as cross-reactivity, as applicable.
(B) Device analytical sensitivity data
generated by testing an adequate
number of samples from individuals
with the target condition including limit
of blank, limit of detection, and limit of
quantification, as applicable.
(C) Device precision/reproducibility
data to evaluate within-run, betweenrun, between-day, between-lot, betweensite, between-reader, within-reader and
total precision, as applicable, using a
panel of samples covering the device
measuring range and/or the relevant
disease categories (e.g. No CIN, CIN1,
CIN2, CIN3, cervical cancer) and testing
in replicates across multiple,
nonconsecutive days.
(D) Device robustness/guardbanding
studies to assess the tolerance ranges for
various critical test and specimen
parameters.
(E) Device stability data, including
real-time stability and shipping stability
under various storage times,
temperatures, and freeze-thaw
conditions.
(F) Data from a clinical study
demonstrating clinical validity using
well-characterized prospectively or
retrospectively obtained clinical
specimens, as appropriate,
representative of the intended use
population. The study must evaluate the
consistency of the diagnosis of CIN, for
example, by comparing the levels of
agreements of diagnoses rendered by
community pathologists to those
rendered by a panel of expert
pathologists. Agreement for each CIN
diagnostic category (e.g., No CIN, CIN1,
CIN2, CIN3, cancer) and for alternate
diagnostic categories (e.g., No CIN, low
grade squamous intraepithelial lesion
(LSIL)-histology, high grade squamous
intraepithelial lesion (HSIL)-histology,
cancer) between reference diagnosis by
expert pathologist and community
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pathologist must be evaluated, as
applicable. In addition, agreements for
CIN binary categories as ≥CIN2 (i.e.,
CIN2 or CIN3 or cancer) and ≤CIN1 (i.e.,
No CIN or CIN1) between reference
diagnosis by expert pathologist with
H&E staining and community
pathologist with H&E staining and
agreements for alternate CIN binary
categories as ≥HSIL-histology (i.e., HSILhistology or cancer) and ≤LSIL-histology
(i.e., No CIN or LSIL-histology) between
reference diagnosis by an expert
pathologist with H&E + [biomarker
specified in paragraph (b)(1)(i) of this
section] and a community pathologist
with H&E + [biomarker specified in
paragraph (b)(1)(i) of this section] must
be evaluated and compared, as
applicable.
(G) The staining performance of the
device as determined by the community
pathologists during review of the study
slides must be evaluated. The staining
performance criteria assessed must
include overall staining acceptability,
background staining acceptability, and
morphology acceptability, as applicable.
(H) Appropriate training requirements
for users, including interpretation
manual, as applicable.
(I) Identification of risk mitigation
elements used by the device, including
a description of all additional
procedures, methods, and practices
incorporated into the instructions for
use that mitigate risks associated with
testing.
(2) The device’s 21 CFR 809.10(b)
compliant labeling must include a
detailed description of the protocol,
including the information described in
paragraph (b)(1)(ii) of this section, as
applicable, and a detailed description of
the performance studies performed and
the summary of the results, including
those that relate to paragraph (b)(1)(ii) of
this section, as applicable.
Dated: December 27, 2017.
Leslie Kux,
Associate Commissioner for Policy.
[FR Doc. 2017–28342 Filed 1–2–18; 8:45 am]
BILLING CODE 4164–01–P
DEPARTMENT OF STATE
22 CFR Parts 35, 103, 127, and 138
[Public Notice 10236]
RIN 1400–AE50
Department of State 2018 Civil
Monetary Penalties Inflationary
Adjustment
Department of State.
Final rule.
AGENCY:
ACTION:
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]]>Agencies
[Federal Register Volume 83, Number 2 (Wednesday, January 3, 2018)]
[Rules and Regulations]
[Pages 232-234]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2017-28342]
=======================================================================
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
21 CFR Part 864
[Docket No. FDA-2017-N-6599]
Medical Devices; Hematology and Pathology Devices; Classification
of a Cervical Intraepithelial Neoplasia Test System
AGENCY: Food and Drug Administration, HHS.
ACTION: Final order.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA or we) is classifying
the cervical intraepithelial neoplasia (CIN) test system into class II
(special controls). The special controls that apply to the device type
are identified in this order and will be part of the codified language
for the CIN test system's classification. We are taking this action
because we have determined that classifying the device into class II
(special controls) will provide a reasonable assurance of safety and
effectiveness of the device. We believe this action will also enhance
patients' access to beneficial innovative devices, in part by reducing
regulatory burdens.
DATES: This order is effective January 3, 2018. The classification was
applicable on March 4, 2017.
FOR FURTHER INFORMATION CONTACT: Steven Tjoe, Center for Devices and
Radiological Health, Food and Drug Administration, 10903 New Hampshire
Ave., Bldg. 66, Rm. 4550, Silver Spring, MD 20993-0002, 301-796-5866,
[email protected].
SUPPLEMENTARY INFORMATION:
I. Background
Upon request, FDA has classified the cervical intraepithelial
neoplasia (CIN) test system as class II (special controls), which we
have determined will provide a reasonable assurance of safety and
effectiveness. In addition, we believe this action will enhance
patients' access to beneficial innovation, in part by reducing
regulatory burdens by placing the device into a lower device class than
the automatic class III assignment.
The automatic assignment of class III occurs by operation of law
and without any action by FDA, regardless of the level of risk posed by
the new device. Any device that was not in commercial distribution
before May 28, 1976, is automatically classified as, and remains
within, class III and requires premarket approval unless and until FDA
takes an action to classify or reclassify the device (see 21 U.S.C.
360c(f)(1)). We refer to these devices as ``postamendments devices''
because they were not in commercial distribution prior to the date of
enactment of the Medical Device Amendments of 1976, which amended the
Federal Food, Drug, and Cosmetic Act (FD&C Act).
FDA may take a variety of actions in appropriate circumstances to
classify or reclassify a device into class I or II. We may issue an
order finding a new device to be substantially equivalent under section
513(i) of the FD&C Act (21 U.S.C. 360c(i)) to a predicate device that
does not require premarket approval. We determine whether a new device
is substantially equivalent to a predicate by means of the procedures
for premarket notification under section 510(k) of the FD&C Act and
part 807 (21 U.S.C. 360(k) and 21 CFR part 807, respectively).
FDA may also classify a device through ``De Novo'' classification,
a common name for the process authorized under section 513(f)(2) of the
[[Page 233]]
FD&C Act. Section 207 of the Food and Drug Administration Modernization
Act of 1997 established the first procedure for De Novo classification
(Pub. L. 105-115). Section 607 of the Food and Drug Administration
Safety and Innovation Act modified the De Novo application process by
adding a second procedure (Pub. L. 112-144). A device sponsor may
utilize either procedure for De Novo classification.
Under the first procedure, the person submits a 510(k) for a device
that has not previously been classified. After receiving an order from
FDA classifying the device into class III under section 513(f)(1) of
the FD&C Act, the person then requests a classification under section
513(f)(2).
Under the second procedure, rather than first submitting a 510(k)
and then a request for classification, if the person determines that
there is no legally marketed device upon which to base a determination
of substantial equivalence, that person requests a classification under
section 513(f)(2) of the FD&C Act.
Under either procedure for De Novo classification, FDA shall
classify the device by written order within 120 days. The
classification will be according to the criteria under section
513(a)(1) of the FD&C Act. Although the device was automatically placed
within class III, the De Novo classification is considered to be the
initial classification of the device.
We believe this De Novo classification will enhance patients'
access to beneficial innovation, in part by reducing regulatory
burdens. When FDA classifies a device into class I or II via the De
Novo process, the device can serve as a predicate for future devices of
that type, including for 510(k)s (see 21 U.S.C. 360c(f)(2)(B)(i)). As a
result, other device sponsors do not have to submit a De Novo request
or premarket approval application in order to market a substantially
equivalent device (see 21 U.S.C. 360c(i), defining ``substantial
equivalence''). Instead, sponsors can use the less-burdensome 510(k)
process, when necessary, to market their device.
II. De Novo Classification
On May 23, 2016, Ventana Medical Systems, Inc., submitted a request
for De Novo classification of the CINtec Histology. FDA reviewed the
request in order to classify the device under the criteria for
classification set forth in section 513(a)(1) of the FD&C Act. We
classify devices into class II if general controls by themselves are
insufficient to provide reasonable assurance of safety and
effectiveness, but there is sufficient information to establish special
controls that, in combination with the general controls, provide
reasonable assurance of the safety and effectiveness of the device for
its intended use (see 21 U.S.C. 360c(a)(1)(B)). After review of the
information submitted in the request, we determined that the device can
be classified into class II with the establishment of special controls.
FDA has determined that these special controls, in addition to the
general controls, will provide reasonable assurance of the safety and
effectiveness of the device.
Therefore, on March 4, 2017, FDA issued an order to the requestor
classifying the device into class II. FDA is codifying the
classification of the device by adding 21 CFR 864.1865. We have named
the generic type of device the cervical intraepithelial neoplasia (CIN)
test system, and it is identified as a device used to detect a
biomarker associated with CIN in human tissues. The device is indicated
as an adjunct test and not to be used as a stand-alone device. The test
results must be interpreted in the context of the patient's clinical
history including, but not limited to, prior and current cervical
biopsy results, Papanicolaou (Pap) test results, human papillomavirus
(HPV) test results, and morphology on hematoxylin and eosin (H&E)
stained sections. This device is not intended to detect the presence of
HPV.
FDA has identified the following risks to health associated
specifically with this type of device and the measures required to
mitigate these risks in table 1.
Table 1--Cervical Intraepithelial Neoplasia (CIN) Test System Risks to
Health and Required Mitigations
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Required mitigations/21 CFR
Identified risks section
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Inaccurate test results, such as false General controls and special
positive or false negative results. controls (1) and (2) (21 CFR
864.1865(b)(1); 21 CFR
864.1865(b)(2)).
Failure to correctly interpret test General controls and special
results can lead to false positive or controls (1) and (2) (21 CFR
false negative results. 864.1865(b)(1); 21 CFR
864.1865(b)(2)).
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FDA has determined that special controls, in combination with the
general controls, address these risks to health and provide reasonable
assurance of safety and effectiveness. For a device to fall within this
classification, and thus avoid automatic classification in class III,
it would have to comply with the special controls named in this final
order. The necessary special controls appear in the regulation codified
by this order. This device is subject to premarket notification
requirements under section 510(k) of the FD&C Act.
III. Analysis of Environmental Impact
The Agency has determined under 21 CFR 25.34(b) that this action is
of a type that does not individually or cumulatively have a significant
effect on the human environment. Therefore, neither an environmental
assessment nor an environmental impact statement is required.
IV. Paperwork Reduction Act of 1995
This final order establishes special controls that refer to
previously approved collections of information found in other FDA
regulations. These collections of information are subject to review by
the Office of Management and Budget (OMB) under the Paperwork Reduction
Act of 1995 (44 U.S.C. 3501-3520). The collections of information in 21
CFR parts 801 and 809, regarding labeling, have been approved under OMB
control number 0910-0485; the collections of information in part 807,
subpart E, regarding premarket notification submissions, have been
approved under OMB control number 0910-0120; the collections of
information in 21 CFR part 814, subparts A through E, regarding
premarket approval, have been approved under OMB control number 0910-
0231; and the collections of information in the guidance document ``De
Novo Classification Process (Evaluation of Automatic Class III
Designation)'' have been approved under OMB control number 0910-0844.
List of Subjects in 21 CFR Part 864
Blood, Medical devices, Packaging and containers.
Therefore, under the Federal Food, Drug, and Cosmetic Act and under
authority delegated to the Commissioner
[[Page 234]]
of Food and Drugs, 21 CFR part 864 is amended as follows:
PART 864--HEMATOLOGY AND PATHOLOGY DEVICES
0
1. The authority citation for part 864 continues to read as follows:
Authority: 21 U.S.C. 351, 360, 360c, 360e, 360j, 360l, 371.
0
2. Add Sec. 864.1865 to subpart B to read as follows:
Sec. 864.1865 Cervical intraepithelial neoplasia (CIN) test system.
(a) Identification. A cervical intraepithelial neoplasia (CIN) test
system is a device used to detect a biomarker associated with CIN in
human tissues. The device is indicated as an adjunct test and not to be
used as a stand-alone device. The test results must be interpreted in
the context of the patient's clinical history including, but not
limited to, prior and current cervical biopsy results, Papanicolaou
(Pap) test results, human papillomavirus (HPV) test results, and
morphology on hematoxylin and eosin (H&E) stained sections. This device
is not intended to detect the presence of HPV.
(b) Classification. Class II (special controls). The special
controls for this device are:
(1) Premarket notification submissions must include the following
information:
(i) The indications for use must specify the biomarker that is
intended to be identified and its adjunct use (e.g., adjunct to
examination of H&E stained slides) to improve consistency in the
diagnosis of CIN.
(ii) Summary of professional society recommendations, as
applicable.
(iii) A detailed device description including:
(A) A detailed description of all test components, including all
provided reagents and required, but not provided, ancillary reagents.
(B) A detailed description of instrumentation and equipment,
including illustrations or photographs of non-standard equipment or
manuals.
(C) If applicable, detailed documentation of the device software,
including, but not limited to, stand-alone software applications and
hardware-based devices that incorporate software.
(D) A detailed description of appropriate positive and negative
controls that are recommended or provided.
(E) Detailed specifications for sample collection, processing, and
storage.
(F) A detailed description of methodology and assay procedure.
(G) A description of the assay cutoff (the medical decision point
between positive and negative) or other relevant criteria that
distinguishes positive and negative results, including the rationale
for the chosen cutoff or other relevant criteria and results supporting
validation of the cutoff.
(H) Detailed specification of the criteria for test results
interpretation and reporting.
(iv) Detailed information demonstrating the performance
characteristics of the device, including:
(A) Analytical specificity studies such as, but not limited to,
antibody characterization (e.g., Western Blot, peptide inhibition
analysis), studies conducted on panels of normal tissues and neoplastic
tissues, interference by endogenous and exogenous substances as well as
cross-reactivity, as applicable.
(B) Device analytical sensitivity data generated by testing an
adequate number of samples from individuals with the target condition
including limit of blank, limit of detection, and limit of
quantification, as applicable.
(C) Device precision/reproducibility data to evaluate within-run,
between-run, between-day, between-lot, between-site, between-reader,
within-reader and total precision, as applicable, using a panel of
samples covering the device measuring range and/or the relevant disease
categories (e.g. No CIN, CIN1, CIN2, CIN3, cervical cancer) and testing
in replicates across multiple, nonconsecutive days.
(D) Device robustness/guardbanding studies to assess the tolerance
ranges for various critical test and specimen parameters.
(E) Device stability data, including real-time stability and
shipping stability under various storage times, temperatures, and
freeze-thaw conditions.
(F) Data from a clinical study demonstrating clinical validity
using well-characterized prospectively or retrospectively obtained
clinical specimens, as appropriate, representative of the intended use
population. The study must evaluate the consistency of the diagnosis of
CIN, for example, by comparing the levels of agreements of diagnoses
rendered by community pathologists to those rendered by a panel of
expert pathologists. Agreement for each CIN diagnostic category (e.g.,
No CIN, CIN1, CIN2, CIN3, cancer) and for alternate diagnostic
categories (e.g., No CIN, low grade squamous intraepithelial lesion
(LSIL)-histology, high grade squamous intraepithelial lesion (HSIL)-
histology, cancer) between reference diagnosis by expert pathologist
and community pathologist must be evaluated, as applicable. In
addition, agreements for CIN binary categories as >=CIN2 (i.e., CIN2 or
CIN3 or cancer) and <=CIN1 (i.e., No CIN or CIN1) between reference
diagnosis by expert pathologist with H&E staining and community
pathologist with H&E staining and agreements for alternate CIN binary
categories as >=HSIL-histology (i.e., HSIL-histology or cancer) and
<=LSIL-histology (i.e., No CIN or LSIL-histology) between reference
diagnosis by an expert pathologist with H&E + [biomarker specified in
paragraph (b)(1)(i) of this section] and a community pathologist with
H&E + [biomarker specified in paragraph (b)(1)(i) of this section] must
be evaluated and compared, as applicable.
(G) The staining performance of the device as determined by the
community pathologists during review of the study slides must be
evaluated. The staining performance criteria assessed must include
overall staining acceptability, background staining acceptability, and
morphology acceptability, as applicable.
(H) Appropriate training requirements for users, including
interpretation manual, as applicable.
(I) Identification of risk mitigation elements used by the device,
including a description of all additional procedures, methods, and
practices incorporated into the instructions for use that mitigate
risks associated with testing.
(2) The device's 21 CFR 809.10(b) compliant labeling must include a
detailed description of the protocol, including the information
described in paragraph (b)(1)(ii) of this section, as applicable, and a
detailed description of the performance studies performed and the
summary of the results, including those that relate to paragraph
(b)(1)(ii) of this section, as applicable.
Dated: December 27, 2017.
Leslie Kux,
Associate Commissioner for Policy.
[FR Doc. 2017-28342 Filed 1-2-18; 8:45 am]
BILLING CODE 4164-01-P
