[Federal Register: August 16, 2007 (Volume 72, Number 158)]
[Proposed Rules]
[Page 45993-45997]
From the Federal Register Online via GPO Access [wais.access.gpo.gov]
[DOCID:fr16au07-34]
[[Page 45993]]
=======================================================================
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
21 CFR Parts 606, 607, 610, and 640
[Docket No. 2007N-0264]
Revisions to the Requirements Applicable to Blood, Blood
Components, and Source Plasma; Companion Document to Direct Final Rule
AGENCY: Food and Drug Administration, HHS.
ACTION: Proposed rule.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA) is proposing to amend
the biologics regulations by removing, revising, or updating specific
regulations applicable to blood, blood components, and Source Plasma to
be more consistent with current practices in the blood industry and to
remove unnecessary or outdated requirements. We are taking this action
as part of our continuing effort to reduce the burden of unnecessary
regulations on industry and to revise outdated regulations without
diminishing public health protection. This proposed rule is a companion
to the direct final rule published elsewhere in this issue of the
Federal Register.
DATES: Submit written or electronic comments by October 30, 2007.
ADDRESSES: You may submit comments, identified by Docket No. 2007N-
0264, by any of the following methods:
Electronic Submissions
Submit electronic comments in the following ways:
Federal eRulemaking Portal: http://www.regulations.gov.
Follow the instructions for submitting comments.
Agency Web site: http://www.fda.gov/dockets/ecomments.
Follow the instructions for submitting comments on the agency Web site.
Written Submissions
Submit written submissions in the following ways:
FAX: 301-827-6870.
Mail/Hand delivery/Courier [For paper, disk, or CD-ROM
submissions]: Division of Dockets Management (HFA-305), Food and Drug
Administration, 5630 Fishers Lane, rm. 1061, Rockville, MD 20852.
To ensure more timely processing of comments, FDA is no longer
accepting comments submitted to the agency by e-mail. FDA encourages
you to continue to submit electronic comments by using the Federal
eRulemaking Portal or the agency Web site, as described previously, in
the ADDRESSES portion of this document under Electronic Submissions.
Instructions: All submissions received must include the agency name
and docket number for this rulemaking. All comments received may be
posted without change to http://www.fda.gov/ohrms/dockets/default.htm,
including any personal information provided. For additional information
on submitting comments, see the ``Comments'' heading of the
SUPPLEMENTARY INFORMATION section of this document.
Docket: For access to the docket to read background documents or
comments received, go to http://www.fda.gov/ohrms/dockets/default.htm
and insert the docket number, found in brackets in the heading of this
document, into the ``Search'' box and follow the prompts and/or go to
the Division of Dockets Management, 5630 Fishers Lane, rm. 1061,
Rockville, MD 20852.
FOR FURTHER INFORMATION CONTACT: Stephen M. Ripley, Center for
Biologics Evaluation and Research (HFM-17), Food and Drug
Administration, 1401 Rockville Pike, Rockville, MD 20852-1448, 301-827-
6210.
SUPPLEMENTARY INFORMATION:
I. Companion Document to Direct Final Rulemaking
This proposed rule is a companion to the direct final rule
published elsewhere in this issue of the Federal Register. This
companion proposed rule provides the procedural framework to finalize
the rule in the event that the direct final rule receives any
significant adverse comments and is withdrawn. The comment period for
this companion proposed rule runs concurrently with the comment period
for the direct final rule. Any comments received under this companion
proposed rule will also be considered as comments regarding the direct
final rule. We are publishing the direct final rule because the rule is
noncontroversial, and we do not anticipate that it will receive any
significant adverse comments.
A significant adverse comment is defined as a comment that explains
why the rule would be inappropriate, including challenges to the rule's
underlying premise or approach, or would be ineffective or unacceptable
without a change. In determining whether an adverse comment is
significant and warrants terminating a direct final rulemaking, we will
consider whether the comment raises an issue serious enough to warrant
a substantive response in a notice-and-comment process in accordance
with section 553 of the Administrative Procedure Act (5 U.S.C. 553).
Comments that are frivolous, insubstantial, or outside the scope of the
rule will not be considered significant or adverse under this
procedure. A comment recommending a regulation change in addition to
those in the rule would not be considered a significant adverse comment
unless the comment states why the rule would be ineffective without
additional change. In addition, if a significant adverse comment
applies to an amendment, paragraph, or section of this rule and that
provision can be severed from the remainder of the rule, we may adopt
as final those provisions of the rule that are not the subject of a
significant adverse comment.
If no significant adverse comment is received in response to the
direct final rule, no further action will be taken related to this
proposed rule. Instead, we will publish a confirmation document, before
the effective date of the direct final rule, confirming that the direct
final rule will go into effect on February 19, 2008. Additional
information about direct rulemaking procedures is set forth in a
guidance published in the Federal Register of November 21, 1997 (62 FR
62466).
II. Legal Authority
FDA is proposing to issue this new rule under the biological
products and communicable diseases provisions of the Public Health
Service Act (PHS Act) (42 U.S.C. 262-264), and the drugs, devices, and
general administrative provisions of the Federal Food, Drug, and
Cosmetic Act (the act) (21 U.S.C. 321, 331, 351-353, 355, 360, 360j,
371, and 374). Under these provisions of the PHS Act and the act, we
have the authority to issue and enforce regulations designed to ensure
that biological products are safe, pure, potent, and properly labeled,
and to prevent the introduction, transmission, and spread of
communicable disease.
III. Highlights of Proposed Rule
FDA is proposing to amend the biologics regulations by removing,
revising, or updating specific regulations applicable to blood, blood
components, and Source Plasma to be more consistent with current
practices in the blood industry and to remove unnecessary or outdated
requirements. We are also issuing these amendments as a direct final
rule because we have concluded that they are noncontroversial and that
there is little likelihood that there will be comments opposing the
rule. Any comment recommending additional changes to these regulations
will not be considered
[[Page 45994]]
to be a ``significant adverse comment'' unless the comment demonstrates
that the change being made in the direct final rule represents a major
departure from current regulations or accepted industry standards, or
cannot be implemented without additional amendments to the regulation.
Below we identify each of the changes included in this proposed rule.
We are proposing to amend 21 CFR 606.3(i) by revising the
definition of ``processing'' to mean any procedure employed after
collection and before ``or after'' compatibility testing of blood. The
current regulation states that processing means any procedure employed
after collection and before compatibility testing of blood. Because
blood components occasionally are further processed after compatibility
testing has been performed, we are proposing this revision to the
definition.
We are proposing to amend 21 CFR 607.65(f) by removing the words
``approved for Medicare reimbursement and'' and replacing with the
words ``that is certified under the Clinical Laboratory Improvement
Amendments of 1988 (42 U.S.C. 263a) and 42 CFR part 493 or has met
equivalent requirements as determined by the Centers for Medicare and
Medicaid Services and which are''. As a result of the Clinical
Laboratory Improvement Amendments of 1988 (CLIA) and the implementing
regulations adopted by the Centers for Medicaid and Medicare Services
(CMS), the inspection regime relied on in a 1983 Memorandum of
Understanding (MOU) between FDA and the Health Care Financing
Administration (HCFA), now CMS, will be modified. Under the CLIA
program, clinical laboratories must be surveyed by CMS (either directly
or through a State survey agency), unless they are located in a CLIA-
approved State, or are accredited by a CMS-approved accreditation
organization. CLIA regulations apply to clinical laboratories
regardless of whether or not the laboratories seek Medicare
participation. FDA is proposing to amend this regulation to make it
consistent with updates in the CMS regulations.
We are proposing to amend 21 CFR 610.53(c) by revising the dating
period in the table for Platelets, Red Blood Cells Deglycerolized, and
Red Blood Cells Frozen. Although the current recommended dating period
would remain unchanged for Platelets and Red Blood Cells
Deglycerolized, we are proposing to add that a different dating period
could apply for these products if so specified in the directions for
use for the blood collecting, processing, and storage system approved
for such use by the Director, Center for Biologics Evaluation and
Research (CBER). This change would allow for flexible dating periods
depending on the type of collecting, processing, and storage system
used. In addition, under Red Blood Cells Frozen, we are proposing to
revise the dating period from 3 years to 10 years, or as specified in
the directions for use for the blood collecting, processing, and
storage system approved for such use by the Director, CBER. This change
would allow for flexible dating periods depending on the type of
collecting, processing, and storage system used.
Under Sec. 640.4(h) (21 CFR 640.4(h)), we are proposing to revise
the temporary storage temperature for blood that is transported from
the donor center to the processing laboratory. We are proposing a range
between 1 and 10[deg] C until the blood arrives at the processing
laboratory. We are proposing this revision to be consistent with 21 CFR
600.15 which allows for shipping temperatures of Whole Blood to be from
1 to 10[deg] C, and for consistency with current industry practice. In
addition, we are proposing to revise the applicability of this
requirement to Whole Blood unless it is to be further processed into
another component, such as Platelets or Red Blood Cells Leukocytes
Reduced. The current regulation applies only to Whole Blood unless the
blood is to be used as a source for Platelets. This change would
clarify that processing Whole Blood into other components, in addition
to Platelets, is acceptable. For Whole Blood that is to be processed
into another component, we are proposing that the blood must be stored
in an environment maintained at a temperature range that is specified
for that component in the directions for use for the blood collecting,
processing, and storage system approved for such use by the Director,
CBER. We are also proposing to replace the term donor ``clinic'' with
donor ``center'' for consistency with Sec. 640.4(b) and current
terminology.
We are proposing to remove and reserve Sec. 640.21(b) (21 CFR
640.21(b)) because this provision is obsolete, as well as proposing to
remove the reference to plasmapheresis in 21 CFR 640.20(b).
Improvements in technology now allow establishments to collect
Platelets by automated methods eliminating the need for the collection
of platelets by manual plasmapheresis. Currently, establishments may
collect Platelets by automated platelet-specific apheresis collection
procedures. We are proposing to amend Sec. 640.21(c) by adding that
plateletpheresis donors must meet the criteria for suitability as
prescribed in 21 CFR 640.3 and 640.63(c)(6), or as described in an
approved biologics license application (BLA) or an approved supplement
to a BLA, and that informed consent must be obtained as prescribed in
21 CFR 640.61. This revision would clarify that registered facilities
must follow the suitability requirements for plateletpheresis donors.
We are proposing to remove and reserve Sec. 640.22(b) (21 CFR
640.22(b)) because this regulation is obsolete. As previously
mentioned, improvements in technology now allow establishments to
collect Platelets by automated methods, eliminating the need for the
collection of platelets by plasmapheresis. Currently, establishments
may collect Platelets by automated platelet-specific apheresis
collection procedures. We are proposing to amend Sec. 640.22(c) by
adding that if plateletpheresis is used, the procedure for collection
must be as prescribed in 21 CFR 640.62--Medical supervision; 21 CFR
640.64--Collection of blood for Source Plasma; and 21 CFR 640.65--
Plasmapheresis, or as described in an approved biologics license
application or an approved supplement to a BLA. This revision would
clarify that registered facilities must follow the collection of source
material requirements for plateletpheresis donors.
We are proposing to amend 21 CFR 640.24(a) to allow Platelets to be
pooled under certain circumstances. That is, Platelets may be pooled if
such processing is specified in the directions for use for the blood
collecting, processing, and storage system for approved such use by the
Director, CBER. We are proposing to amend the regulation to provide
flexibility depending on the type of collecting, processing, and
storage system used.
We are proposing to amend 21 CFR 640.25(b)(2) by revising the pH
level from ``6.0'' to ``6.2'' for consistency with current industry
practice. Studies have shown that a lower pH may adversely affect
platelet function (Refs. 1 and 2).
We are proposing to amend 21 CFR 640.30(a) by revising the term
``product,'' to ``component,'' for consistency with current terminology
of the proper name. We are also proposing to add an alternative
definition of Plasma, namely, ``The fluid portion of human blood
intended for intravenous use which is prepared by apheresis methods as
specified in the directions for use for the blood collecting,
processing, and storage system including closed and open systems.'' We
are proposing this change because
[[Page 45995]]
Plasma is now collected by other methods, such as apheresis collection,
in addition to being collected as a byproduct of Whole Blood
collection.
We are proposing to amend 21 CFR 640.32(a) to add that a different
storage temperature may be used for Whole Blood intended for further
manufacturing into Plasma, Fresh Frozen Plasma, or Liquid Plasma. Any
different storage temperature would be specified in the directions for
use for the blood collecting, processing, and storage system. This
change would allow for flexible storage temperatures depending on the
particular type of system used.
We are proposing to amend 21 CFR 640.34(b) by adding the phrase
``or collected by an apheresis procedure'' in the second sentence to
clarify that this section also applies to plasma collected by aphersis
procedures. We would require that fresh frozen plasma using the
apheresis procedure be prepared from blood collected by a single
uninterrupted venipuncture with minimal damage to, and minimal
manipulation of, the donor's tissue.
We are proposing to amend Sec. 640.64(b) (21 CFR 640.64(b)) by
removing the second sentence that states, ``The amount of anticoagulant
required for the quantity of blood to be collected shall be in the
blood container when it is sterilized.'' We are proposing to remove
this sentence because of technological advances. Now, the anticoagulant
does not always have to be in the collection set. The anticoagulant can
be connected by a ``sterile docking'' procedure or attached separately,
as is the case with automated apheresis collection. We are also
proposing to amend Sec. 640.64(c) by removing the specific
anticoagulant solution formulas and indicating that the anticoagulant
solutions must be compounded and used according to a formula approved
by the Director, CBER. We have determined that it is unnecessary to
provide specific formulae for anticoagulant solutions in the
regulations, and that manufacturers should be able to use any
anticoagulant approved by the FDA for such use by the manufacturer.
We have also revised the above regulations, where applicable, by
using ``must'' or ``is'' instead of ``shall,'' depending on the
circumstances. We have made these revisions for plain language
purposes. These editorial changes are for clarity only and do not
change the substance of the requirements. We will continue to make
these changes in other applicable regulations as they are revised in
future rulemakings. In addition, we will continue to make the change
from ``product'' to ``component'' in other applicable regulations as
they are revised in future rulemakings.
IV. Analysis of Impacts
A. Review Under Executive Order 12866, the Regulatory Flexibility Act,
and the Unfunded Mandates Act of 1995
FDA has examined the impacts of the proposed rule under Executive
Order 12866 and the Regulatory Flexibility Act (5 U.S.C. 601-612), and
the Unfunded Mandates Reform Act of 1995 (Public Law 104-4). Executive
Order 12866 directs agencies to assess all costs and benefits of
available regulatory alternatives and, when regulation is necessary, to
select regulatory approaches that maximize net benefits (including
potential economic, environmental, public health and safety, and other
advantages; distributive impacts; and equity). The agency believes that
this proposed rule is not a significant regulatory action as defined by
the Executive order.
The Regulatory Flexibility Act requires agencies to analyze
regulatory options that would minimize any significant impact of a rule
on small entities. Because the proposed rule amendments have no
compliance costs and do not result in any new requirements, the agency
certifies that the proposed rule will not have a significant economic
impact on a substantial number of small entities.
Section 202(a) of the Unfunded Mandates Reform Act of 1995 requires
that agencies prepare a written statement, which includes an assessment
of anticipated costs and benefits, before proposing ``any rule that
includes any Federal mandate that may result in the expenditure by
State, local, and tribal governments, in the aggregate, or by the
private sector, of $100,000,000 or more (adjusted annually for
inflation) in any one year.'' The current threshold after adjustment
for inflation is $122 million, using the most current (2005) Implicit
Price Deflator for the Gross Domestic Product. FDA does not expect this
proposed rule to result in any 1-year expenditure that would meet or
exceed this amount.
B. Environmental Impact
The agency has determined, under 21 CFR 25.31(h), 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.
C. Federalism
FDA has analyzed this proposed rule in accordance with the
principles set forth in Executive Order 13132. FDA has determined that
the proposed rule does not contain policies that 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. Accordingly,
the agency has concluded that the proposed rule does not contain
policies that have federalism implications as defined in the Executive
order and, consequently, a federalism summary impact statement is not
required.
V. Paperwork Reduction Act of 1995
FDA tentatively concludes that this proposed rule contains no
collection of information. Therefore clearance by OMB under the
Paperwork Reduction Act of 1995 is not required.
VI. Request for Comments
Interested persons may submit to the Division of Dockets Management
(see ADDRESSES) written or electronic comments regarding this document.
Submit a single copy of electronic comments or two paper copies of any
mailed comments, except that individuals may submit one paper copy.
Comments are to be identified with the docket number found in brackets
in the heading of this document. Received comments may be seen in the
Division of Dockets Management between 9 a.m. and 4 p.m., Monday
through Friday.
VII. References
The following references have been placed on display in the
Division of Dockets Management (see ADDRESSES), and may be seen by
interested persons between 9 a.m. and 4 p.m., Monday through Friday.
1. Scott Murphy, ``Platelet Storage for Transfusion,'' Seminars
in Hematology, 22(3): 165-177, July 1985.
2. L. Dumont and T. VandenBroeke, ``Seven-Day Storage of
Apheresis Platelets Report of an In Vitro Study,'' 43: 143-150,
Transfusion, February 2003.
List of Subjects
21 CFR Part 606
Blood, Labeling, Laboratories, Reporting and recordkeeping
requirements.
21 CFR Part 607
Blood.
21 CFR Part 610
Biologics, Labeling, Reporting and recordkeeping requirements.
[[Page 45996]]
21 CFR Part 640
Blood, Labeling, Reporting and recordkeeping requirements.
Therefore, under the Federal Food, Drug, and Cosmetic Act and the
Public Health Service Act, and under authority delegated by the
Commissioner of Food and Drugs, it is proposed that 21 CFR parts 606,
607, 610, and 640 be amended as follows:
PART 606--CURRENT GOOD MANUFACTURING PRACTICE FOR BLOOD AND BLOOD
COMPONENTS
1. The authority citation for 21 CFR part 606 continues to read as
follows:
Authority: 21 U.S.C. 321, 331, 351, 352, 355, 360, 360j, 371,
374; 42 U.S.C. 216, 262, 263a, 264.
2. Section 606.3 is amended by revising paragraph (i) to read as
follows:
Sec. 606.3 Definitions.
* * * * *
(i) Processing means any procedure employed after collection and
before or after compatibility testing of blood, and includes the
identification of a unit of donor blood, the preparation of components
from such unit of donor blood, serological testing, labeling and
associated recordkeeping.
* * * * *
PART 607--ESTABLISHMENT REGISTRATION AND PRODUCT LISTING FOR
MANUFACTURERS OF HUMAN BLOOD AND BLOOD PRODUCTS
3. The authority citation for 21 CFR part 607 continues to read as
follows:
Authority: 21 U.S.C. 321, 331, 351, 352, 355, 360, 371, 374,
381, 393; 42 U.S.C. 262, 264, 271.
4. Section 607.65 is amended by revising the first sentence in
paragraph (f) to read as follows:
Sec. 607.65 Exemptions for blood product establishments.
* * * * *
(f) Transfusion services which are a part of a facility that is
certified under the Clinical Laboratory Improvement Amendments of 1988
(42 U.S.C. 263a) and 42 CFR part 493 or has met equivalent requirements
as determined by the Centers for Medicare and Medicaid Services and
which are engaged in the compatibility testing and transfusion of blood
and blood components, but which neither routinely collect nor process
blood and blood components. * * *
PART 610--GENERAL BIOLOGICAL PRODUCTS STANDARDS
5. The authority citation for 21 CFR part 610 continues to read as
follows:
Authority: 21 U.S.C. 321, 331, 351, 352, 353, 355, 360, 360c,
360d, 360h, 360i, 371, 372, 374, 381; 42 U.S.C. 216, 262, 263, 263a,
264.
6. Section 610.53 is amended in paragraph (c) in the table by
revising the entries for Platelets, Red Blood Cells Deglycerolized, and
Red Blood Cells Frozen to read as follows:
Sec. 610.53 Dating periods for licensed biological products.
* * * * *
(c) * * *
----------------------------------------------------------------------------------------------------------------
A B C D
----------------------------------------------------------------------------------------------------------------
Product Manufacturer's storage Manufacturer's storage Dating period after leaving
period 1 to 5[deg] C period 0[deg] C or manufacturer's storage when stored at 2
(unless otherwise colder (unless to 8[deg] C (unless otherwise stated)
stated). otherwise stated).
----------------------------------------------------------------------------------------------------------------
* * * * * * *
----------------------------------------------------------------------------------------------------------------
Platelets Not applicable......... do..................... 72 hours from time of collection of
source blood, provided labeling
recommends storage at 20 to 24[deg] C or
between 1 and 6[deg] C, or as specified
in the directions for use for the blood
collecting, processing, and storage
system approved for such use by the
Director, Center for Biologics
Evaluation and Research (CBER).
----------------------------------------------------------------------------------------------------------------
* * * * * * *
----------------------------------------------------------------------------------------------------------------
Red Blood Cells do..................... do..................... 24 hours after removal from storage at
Deglycerolized 65[deg] C or colder, provided labeling
recommends storage between 1 and 6[deg]
C, or as specified in the directions for
use for the blood collecting,
processing, and storage system approved
for such use by the Director, CBER.
----------------------------------------------------------------------------------------------------------------
Red Blood Cells do..................... do..................... 10 years from date of collection of
Frozen source blood, provided labeling
recommends storage at 65[deg] C or
colder, or as specified in the
directions for use for the blood
collecting, processing, and storage
system approved for such use by the
Director, CBER.
----------------------------------------------------------------------------------------------------------------
* * * * *
PART 640--ADDITIONAL STANDARDS FOR HUMAN BLOOD AND BLOOD PRODUCTS
7. The authority citation for 21 CFR part 640 continues to read as
follows:
Authority: 21 U.S.C. 321, 351, 352, 353, 355, 360, 371; 42
U.S.C. 216, 262, 263, 263a, 264.
8. Section 640.4 is amended by revising paragraph (h) to read as
follows:
Sec. 640.4 Collection of the blood.
* * * * *
(h) Storage. Whole blood must be placed in storage at a temperature
between 1 and 6[deg] C immediately after collection unless the blood is
to be further processed into another component or the blood must be
transported from the donor center to the processing laboratory. If
transported, the blood must be placed in temporary storage having
sufficient refrigeration capacity to cool the blood continuously at a
temperature range between 1 and 10[deg] C until arrival at the
processing laboratory. At the processing laboratory, the blood must be
stored at a temperature between 1 and 6[deg] C. Blood from which a
component is to be prepared must be held in an environment maintained
at a temperature range specified for that
[[Page 45997]]
component in the directions for use for the blood collecting,
processing, and storage system approved for such use by the Director,
CBER.
9. Section 640.20 is amended by revising paragraph (b) to read as
follows:
Sec. 640.20 Platelets.
* * * * *
(b) Source. The source material for Platelets is plasma which may
be obtained by whole blood collection or by plateletpheresis.
10. Section 640.21 is amended by removing and reserving paragraph
(b) and revising paragraph (c) to read as follows:
Sec. 640.21 Suitability of donors.
* * * * *
(b) [Reserved]
(c) Plateletpheresis donors must meet the criteria for suitability
as prescribed in Sec. Sec. 640.3 and 640.63(c)(6), or as described in
an approved biologics license application (BLA) or an approved
supplement to a BLA. Informed consent must be obtained as prescribed in
Sec. 640.61.
11. Section 640.22 is amended by removing and reserving paragraph
(b) and revising paragraph (c) to read as follows:
Sec. 640.22 Collection of source material.
* * * * *
(b) [Reserved]
(c) If plateletpheresis is used, the procedure for collection must
be as prescribed in Sec. Sec. 640.62, 640.64 (except paragraph (c)),
and 640.65, or as described in an approved biologics license
application (BLA) or an approved supplement to a BLA.
* * * * *
12. Section 640.24 is amended by revising paragraph (a) to read as
follows:
Sec. 640.24 Processing.
(a) Separation of plasma and platelets and resuspension of the
platelets must be in a closed system. Platelets must not be pooled
during processing unless the platelets are pooled as specified in the
directions for use for the blood collecting, processing, and storage
system approved for such use by the Director, Center for Biologics
Evaluation and Research.
* * * * *
Sec. 640.25 [Amended]
13. Section 640.25 is amended in paragraph (b)(2) by removing
``6.0'' and adding in its place ``6.2''.
14. Section 640.30 is amended by revising paragraph (a) to read as
follows:
Sec. 640.30 Plasma.
(a) Proper name and definition. The proper name of this component
is Plasma. The component is defined as:
(1) The fluid portion of one unit of human blood intended for
intravenous use which is collected in a closed system, stabilized
against clotting, and separated from the red cells; or
(2) The fluid portion of human blood intended for intravenous use
which is prepared by apheresis methods as specified in the directions
for use for the blood collecting, processing, and storage system
including closed and open systems.
* * * * *
15. Section 640.32 is amended by revising paragraph (a) to read as
follows:
Sec. 640.32 Collection of source material.
(a) Whole Blood must be collected, transported, and stored as
prescribed in Sec. 640.4. When whole blood is intended for Plasma,
Fresh Frozen Plasma, and Liquid Plasma, until the plasma is removed,
the whole blood must be maintained at a temperature between 1 and
6[deg] C or as specified in the directions for use for the blood
collecting, processing, and storage system approved for such use by the
Director, Center for Biologics Evaluations and Research. Whole blood
intended for Platelet Rich Plasma must be maintained as prescribed in
Sec. 640.24 until the plasma is removed. The red blood cells must be
placed in storage at a temperature between 1 and 6[deg] C immediately
after the plasma is separated.
* * * * *
16. Section 640.34 is amended by revising the second sentence in
paragraph (b) to read as follows:
Sec. 640.34 Processing.
* * * * *
(b) Fresh Frozen Plasma. * * * The plasma must be separated from
the red blood cells or collected by an apheresis procedure, and placed
in a freezer within 8 hours or within the timeframe specified in the
directions for use for the blood collecting, processing, and storage
system, and stored at 18[deg] C or colder.
* * * * *
17. Section 640.64 is amended by revising paragraphs (b) and (c) to
read as follows:
Sec. 640.64 Collection of blood for source plasma.
* * * * *
(b) Blood containers. Blood containers and donor sets must be
pyrogen-free, sterile, and identified by lot number.
(c) The anticoagulant solution. The anticoagulant solution must be
sterile and pyrogen-free. Anticoagulant solutions must be compounded
and used according to a formula that has been approved for the
applicant by the Director, Center for Biologics Evaluation and
Research.
* * * * *
Dated: July 23, 2007.
Jeffrey Shuren,
Assistant Commissioner for Policy.
[FR Doc. E7-15942 Filed 8-15-07; 8:45 am]
BILLING CODE 4160-01-S