Amprotec provides
this information for the purpose of supporting you in the design of your food
grade tank installations.
21 Code of Federal Regulations Provided By the
US FDA
Parts 210 and 211
Part 210 - CURRENT GOOD MANUFACTURING PRACTICE IN
MANUFACTURING, PROCESSING, PACKING, OR HOLDING OF DRUGS; GENERAL PART
211 - CURRENT GOOD MANUFACTURING PRACTICE FOR FINISHED
PHARMACEUTICALS
Part 210 - CURRENT GOOD MANUFACTURING PRACTICE IN MANUFACTURING,
PROCESSING, PACKING, OR HOLDING OF DRUGS; GENERAL
210.1 Status of current good manufacturing practice
regulations.
210.2 Applicability of current good manufacturing practice
regulations.
210.3 Definitions.
AUTHORITY: Secs. 201, 501, 502, 505, 506, 507, 512, 701, 704 of the
Federal Food, Drug, and Cosmetic Act (21 U.S.C. 321, 351, 352, 355,
356, 357, 360b, 371, 374).
SOURCE: 43 FR 45076, Sept. 29, 1978, unless otherwise noted.
§ 210.1 Status of current good manufacturing
practice regulations.
(a) The regulations set forth in this part and in Parts 211 through
226 of this chapter contain the minimum current good manufacturing
practice for methods to be used in, and the facilities or controls to
be used for, the manufacture, processing, packing, or holding of a
drug to assure that such drug meets the requirements of the act as to
safety, and has the identity and strength and meets the quality and
purity characteristics that it purports or is represented to possess.
(b) The failure to comply with any regulation set forth in this
part and in Parts 211 through 226 of this chapter in the manufacture,
processing, packing, or holding of a drug shall render such drug to be
adulterated under section 501(a)(2)(B) of the act and such drug, as
well as the person who is responsible for the failure to comply, shall
be subject to regulatory action.
§ 210.2 Applicability of current good
manufacturing practice regulations.
(a) The regulations in this part and in Parts 211 through 226 of
this chapter as they may pertain to a drug and in Parts 600 through
680 of this chapter as they may pertain to a biological product for
human use, shall be considered to supplement, not supersede, each
other, unless the regulations explicitly provide otherwise. In the
event that it is impossible to comply with all applicable regulations
in these parts, the regulations specifically applicable to the drug in
question shall supersede the more general.
(b) If a person engages in only some operations subject to the
regulations in this part and in Parts 211 through 226 and Parts 600
through 680 of this chapter, and not in others, that person need only
comply with those regulations applicable to the operations in which he
or she is engaged.
§ 210.3 Definitions.
(a) The definitions and interpretations contained in section 201 of
the act shall be applicable to such terms when used in this part and
in Parts 211 through 226 of this chapter.
(b) The following definitions of terms apply to this part and to
Parts 211 through 226 of this chapter.
(1) Act means the Federal Food, Drug, and Cosmetic Act, as
amended (21 U.S.C. 301 et seq.).
(2) Batch means a specific quantity of a drug or other
material that is intended to have uniform character and quality,
within specified limits, and is produced according to a single
manufacturing order during the same cycle of manufacture.
(3) Component means any ingredient intended for use in the
manufacture of a drug product, including those that may not appear in
such drug product.
(4) Drug product means a finished dosage form, for example,
tablet, capsule, solution, etc., that contains an active drug
ingredient generally, but not necessarily, in association with
inactive ingredients. The term also includes a finished dosage form
that does not contain an active ingredient but is intended to be used
as a placebo.
(5) Fiber means any particulate contaminant with a length at
least three times greater than its width.
(6) Non-fiber-releasing filter means any filter, which after
any appropriate pretreatment such as washing or flushing, will not
release fibers into the component or drug product that is being
filtered. All filters composed of asbestos are deemed to be
fiber-releasing filters.
(7) Active ingredient means any component that is intended
to furnish pharmacological activity or other direct effect in the
diagnosis, cure, mitigation, treatment, or prevention of disease, or
to affect the structure or any function of the body of man or other
animals. The term includes those components that may undergo chemical
change in the manufacture of the drug product and be present in the
drug product in a modified form intended to furnish the specified
activity or effect.
(8) Inactive ingredient means any component other than an
``active ingredient.''
(9) In-process material means any material fabricated,
compounded, blended, or derived by chemical reaction that is produced
for, and used in, the preparation of the drug product.
(10) Lot means a batch, or a specific identified portion of
a batch, having uniform character and quality within specified limits;
or, in the case of a drug product produced by continuous process, it
is a specific identified amount produced in a unit of time or quantity
in a manner that assures its having uniform character and quality
within specified limits.
(11) Lot number, control number, or batch number means any
distinctive combination of letters, numbers, or symbols, or any
combination of them, from which the complete history of the
manufacture, processing, packing, holding, and distribution of a batch
or lot of drug product or other material can be determined.
(12) Manufacture, processing, packing, or holding of a drug
product includes packaging and labeling operations, testing, and
quality control of drug products.
(13) The term medicated feed means any Type B or Type C
medicated feed as defined in 558.3 of this chapter. The feed contains
one or more drugs as defined in section 201(g) of the act. The
manufacture of medicated feeds is subject to the requirements of Part
225 of this chapter.
(14) The term medicated premix means a Type A medicated
article as defined in 558.3 of this chapter. The article contains one
or more drugs as defined in section 201(g) of the act. The manufacture
of medicated premixes is subject to the requirements of Part 226 of
this chapter.
(15) Quality control unit means any person or organizational
element designated by the firm to be responsible for the duties
relating to quality control.
(16) Strength means:
(I) The concentration of the drug substance (for example,
weight/weight, weight/volume, or unit dose/volume basis), and/or
(ii) The potency, that is, the therapeutic activity of the drug
product as indicated by appropriate laboratory tests or by adequately
developed and controlled clinical data (expressed, for example, in
terms of units by reference to a standard).
(17) Theoretical yield means the quantity that would be
produced at any appropriate phase of manufacture, processing, or
packing of a particular drug product, based upon the quantity of
components to be used, in the absence of any loss or error in actual
production.
(18) Actual yield means the quantity that is actually
produced at any appropriate phase of manufacture, processing, or
packing of a particular drug product.
(19) Percentage of theoretical yield means the ratio of the
actual yield (at any appropriate phase of manufacture, processing, or
packing of a particular drug product) to the theoretical yield (at the
same phase), stated as a percentage.
(20) Acceptance criteria means the product specifications
and acceptance/rejection criteria, such as acceptable quality level
and unacceptable quality level, with an associated sampling plan, that
are necessary for making a decision to accept or reject a lot or batch
(or any other convenient subgroups of manufactured units).
(21) Representative sample means a sample that consists of a
number of units that are drawn based on rational criteria such as
random sampling and intended to assure that the sample accurately
portrays the material being sampled.
(22) Gang-printed labeling means labeling derived from a
sheet of material on which more than one item of labeling is printed.
[43 FR 45076, Sept. 29, 1978, as amended at 51 FR 7389, Mar. 3,
1986; 58 FR 41353, Aug. 3, 1993]
EFFECTIVE DATE NOTE: At 58 FR 41353, Aug. 8, 1993, 210.3 was
amended by adding paragraph (b)(22) effective Aug. 3, 1994.
Part 211 -CURRENT GOOD MANUFACTURING
PRACTICE FOR FINISHED PHARMACEUTICALS
(21 CFR Part 211 As of April, 1996)
Authority: Secs. 201, 501, 502, 505, 506, 507, 512, 701, 704 of the
Federal Food, Drug, and Cosmetic Act (21 U.S.C. 321, 351, 352, 355,
356, 357, 360b, 371, 374).
Source: 43 FR 45077, Sept. 29, 1978, unless otherwise noted.
PART 211 - CURRENT GOOD MANUFACTURING PRACTICE FOR FINISHED
PHARMACEUTICALS
Subpart A--General Provisions
§ 211.1 - Scope.
§ 211.3 - Definitions.
Subpart B--Organization and Personnel
§ 211.22 - Responsibilities of quality control unit.
§ 211.25 - Personnel qualifications.
§ 211.28 - Personnel responsibilities.
§ 211.34 - Consultants.
Subpart A-General Provisions
§ 211.1 Scope
(a) The regulations in this part contain the minimum current good
manufacturing practice for preparation of drug products for
administration to humans or animals.
(b) The current good manufacturing practice regulations in this
chapter, as they pertain to drug products, and in parts 600 through
680 of this chapter, as they pertain to biological products for human
use, shall be considered to supplement, not supersede, the regulations
in this part unless the regulations explicitly provide otherwise. In
the event it is impossible to comply with applicable regulations both
in this part and in other parts of this chapter or in parts 600
through 680 of this chapter, the regulation specifically applicable to
the drug product in question shall supersede the regulation in this
part.
(c) Pending consideration of a proposed exemption, published in the
Federal Register of September 29, 1978, the requirements in this part
shall not be enforced for OTC drug products if the products and all
their ingredients are ordinarily marketed and consumed as human foods,
and which products may also fall within the legal definition of drugs
by virtue of their intended use. Therefore, until further notice,
regulations under part 110 of this chapter, and where applicable,
parts 113 to 129 of this chapter, shall be applied in determining
whether these OTC drug products that are also foods are manufactured,
processed, packed, or held under current good manufacturing practice.
§ 211.3 Definitions.
The definitions set forth in § 210.3 of this chapter apply in this
part.
Subpart B-Organization and Personnel
§ 211.22 Responsibilities of quality
control unit.
(a) There shall be a quality control unit that shall have the
responsibility and authority to approve or reject all components, drug
product containers, closures, in-process materials, packaging
material, labeling, and drug products, and the authority to review
production records to assure that no errors have occurred or, if
errors have occurred, that they have been fully investigated. The
quality control unit shall be responsible for approving or rejecting
drug products manufactured, processed, packed, or held under contract
by another company.
(b) Adequate laboratory facilities for the testing and approval (or
rejection) of components, drug product containers, closures, packaging
materials, in-process materials, and drug products shall be available
to the quality control unit.
(c) The quality control unit shall have the responsibility for
approving or rejecting all procedures or specifications impacting on
the identity, strength, quality, and purity of the drug product.
(d) The responsibilities and procedures applicable to the quality
control unit shall be in writing; such written procedures shall be
followed.
§ 211.25 Personnel qualifications.
(a) Each person engaged in the manufacture, processing, packing, or
holding of a drug product shall have education, training, and
experience, or any combination thereof, to enable that person to
perform the assigned functions. Training shall be in the particular
operations that the employee performs and in current good
manufacturing practice (including the current good manufacturing
practice regulations in this chapter and written procedures required
by these regulations) as they relate to the employee's functions.
Training in current good manufacturing practice shall be conducted by
qualified individuals on a continuing basis and with sufficient
frequency to assure that employees remain familiar with CGMP
requirements applicable to them.
(b) Each person responsible for supervising the manufacture,
processing, packing, or holding of a drug product shall have the
education, training, and experience, or any combination thereof, to
perform assigned functions in such a manner as to provide assurance
that the drug product has the safety, identity, strength, quality, and
purity that it purports or is represented to possess.
(c) There shall be an adequate number of qualified personnel to
perform and supervise the manufacture, processing, packing, or holding
of each drug product.
§ 211.28 Personnel responsibilities.
(a) Personnel engaged in the manufacture, processing, packing, or
holding of a drug product shall wear clean clothing appropriate for
the duties they perform. Protective apparel, such as head, face, hand,
and arm coverings, shall be worn as necessary to protect drug products
from contamination.
(b) Personnel shall practice good sanitation and health habits.
(c) Only personnel authorized by supervisory personnel shall enter
those areas of the buildings and facilities designated as
limited-access areas.
(d) Any person shown at any time (either by medical examination or
supervisory observation) to have an apparent illness or open lesions
that may adversely affect the safety or quality of drug products shall
be excluded from direct contact with components, drug product
containers, closures, in-process materials, and drug products until
the condition is corrected or determined by competent medical
personnel not to jeopardize the safety or quality of drug products.
All personnel shall be instructed to report to supervisory personnel
any health conditions that may have an adverse effect on drug
products.
§ 211.34 Consultants.
Consultants advising on the manufacture, processing, packing, or
holding of drug products shall have sufficient education, training,
and experience, or any combination thereof, to advise on the subject
for which they are retained. Records shall be maintained stating the
name, address, and qualifications of any consultants and the type of
service they provide.
Subpart C-Buildings and Facilities
§ 211.42 Design and construction features.
(a) Any building or buildings used in the manufacture, processing,
packing, or holding of a drug product shall be of suitable size,
construction and location to facilitate cleaning, maintenance, and
proper operations.
(b) Any such building shall have adequate space for the orderly
placement of equipment and materials to prevent mixups between
different components, drug product containers, closures, labeling,
in-process materials, or drug products, and to prevent contamination.
The flow of components, drug product containers, closures, labeling,
in-process materials, and drug products through the building or
buildings shall be designed to prevent contamination.
(c) Operations shall be performed within specifically defined areas
of adequate size. There shall be separate or defined areas for the
firm's operations to prevent contamination or mixups as follows:
(1) Receipt, identification, storage, and withholding from use of
components, drug product containers, closures, and labeling, pending
the appropriate sampling, testing, or examination by the quality
control unit before release for manufacturing or packaging;
(2) Holding rejected components, drug product containers, closures,
and labeling before disposition;
(3) Storage of released components, drug product containers,
closures, and labeling;
(4) Storage of in-process materials;
(5) Manufacturing and processing operations;
(6) Packaging and labeling operations;
(7) Quarantine storage before release of drug products;
(8) Storage of drug products after release;
(9) Control and laboratory operations;
(10) Aseptic processing, which includes as appropriate:
(I) Floors, walls, and ceilings of smooth, hard surfaces that are
easily cleanable;
(ii) Temperature and humidity controls;
(iii) An air supply filtered through high-efficiency particulate
air filters under positive pressure, regardless of whether flow is
laminar or nonlaminar;
(iv) A system for monitoring environmental conditions;
(v) A system for cleaning and disinfecting the room and equipment
to produce aseptic conditions;
(vi) A system for maintaining any equipment used to control the
aseptic conditions.
(d) Operations relating to the manufacture, processing, and packing
of penicillin shall be performed in facilities separate from those
used for other drug products for human use.
[43 FR 45077, Sept. 29, 1978, as amended at 60 FR 4091, Jan. 20,
1995]
§ 211.44 Lighting.
Adequate lighting shall be provided in all areas.
§ 211.46 Ventilation, air filtration, air
heating and cooling.
(a) Adequate ventilation shall be provided.
(b) Equipment for adequate control over air pressure,
micro-organisms, dust, humidity, and temperature shall be provided
when appropriate for the manufacture, processing, packing, or holding
of a drug product.
(c) Air filtration systems, including prefilters and particulate
matter air filters, shall be used when appropriate on air supplies to
production areas. If air is recirculated to production areas, measures
shall be taken to control recirculation of dust from production. In
areas where air contamination occurs during production, there shall be
adequate exhaust systems or other systems adequate to control
contaminants.
(d) Air-handling systems for the manufacture, processing, and
packing of penicillin shall be completely separate from those for
other drug products for human use.
§ 211.48 Plumbing.
(a) Potable water shall be supplied under continuous positive
pressure in a plumbing system free of defects that could contribute
contamination to any drug product. Potable water shall meet the
standards prescribed in the Environmental Protection Agency's Primary
Drinking Water Regulations set forth in 40 CFR part 141. Water not
meeting such standards shall not be permitted in the potable water
system.
(b) Drains shall be of adequate size and, where connected directly
to a sewer, shall be provided with an air break or other mechanical
device to prevent back-siphonage.
[43 FR 45077, Sept. 29, 1978, as amended at 48 FR 11426, Mar. 18,
1983]
§ 211.50 Sewage and refuse.
Sewage, trash, and other refuse in and from the building and
immediate premises shall be disposed of in a safe and sanitary manner.
§ 211.52 Washing and toilet facilities.
Adequate washing facilities shall be provided, including hot and
cold water, soap or detergent, air driers or single-service towels,
and clean toilet facilities easily accessible to working areas.
§ 211.56 Sanitation.
(a) Any building used in the manufacture, processing, packing, or
holding of a drug product shall be maintained in a clean and sanitary
condition, Any such building shall be free of infestation by rodents,
birds, insects, and other vermin (other than laboratory animals).
Trash and organic waste matter shall be held and disposed of in a
timely and sanitary manner.
(b) There shall be written procedures assigning responsibility for
sanitation and describing in sufficient detail the cleaning schedules,
methods, equipment, and materials to be used in cleaning the buildings
and facilities; such written procedures shall be followed.
(c) There shall be written procedures for use of suitable
rodenticides, insecticides, fungicides, fumigating agents, and
cleaning and sanitizing agents. Such written procedures shall be
designed to prevent the contamination of equipment, components, drug
product containers, closures, packaging, labeling materials, or drug
products and shall be followed. Rodenticides, insecticides, and
fungicides shall not be used unless registered and used in accordance
with the Federal Insecticide, Fungicide, and Rodenticide Act (7 U.S.C.
135).
(d) Sanitation procedures shall apply to work performed by
contractors or temporary employees as well as work performed by
full-time employees during the ordinary course of operations.
§ 211.58 Maintenance.
Any building used in the manufacture, processing, packing, or
holding of a drug product shall be maintained in a good state of
repair.
§ 211.63 Equipment design, size, and
location.
Equipment used in the manufacture, processing, packing, or holding
of a drug product shall be of appropriate design, adequate size, and
suitably located to facilitate operations for its intended use and for
its cleaning and maintenance.
§ 211.65 Equipment construction.
(a) Equipment shall be constructed so that surfaces that contact
components, in-process materials, or drug products shall not be
reactive, additive, or absorptive so as to alter the safety, identity,
strength, quality, or purity of the drug product beyond the official
or other established requirements.
(b) Any substances required for operation, such as lubricants or
coolants, shall not come into contact with components, drug product
containers, closures, in-process materials, or drug products so as to
alter the safety, identity, strength, quality, or purity of the drug
product beyond the official or other established requirements.
§ 211.67 Equipment cleaning and
maintenance.
(a) Equipment and utensils shall be cleaned, maintained, and
sanitized at appropriate intervals to prevent malfunctions or
contamination that would alter the safety, identity, strength,
quality, or purity of the drug product beyond the official or other
established requirements.
(b) Written procedures shall be established and followed for
cleaning and maintenance of equipment, including utensils, used in the
manufacture, processing, packing, or holding of a drug product. These
procedures shall include, but are not necessarily limited to, the
following:
(1) Assignment of responsibility for cleaning and maintaining
equipment;
(2) Maintenance and cleaning schedules, including, where
appropriate, sanitizing schedules;
(3) A description in sufficient detail of the methods, equipment,
and materials used in cleaning and maintenance operations, and the
methods of disassembling and reassembling equipment as necessary to
assure proper cleaning and maintenance;
(4) Removal or obliteration of previous batch identification;
(5) Protection of clean equipment from contamination prior to use;
(6) Inspection of equipment for cleanliness immediately before use.
(c) Records shall be kept of maintenance, cleaning, sanitizing, and
inspection as specified in §§ 211.180 and 211.182.
§ 211.68 Automatic, mechanical, and
electronic equipment.
(a) Automatic, mechanical, or electronic equipment or other types
of equipment, including computers, or related systems that will
perform a function satisfactorily, may be used in the manufacture,
processing, packing, and holding of a drug product. If such equipment
is so used, it shall be routinely calibrated, inspected, or checked
according to a written program designed to assure proper performance.
Written records of those calibration checks and inspections shall be
maintained.
(b) Appropriate controls shall be exercised over computer or
related systems to assure that changes in master production and
control records or other records are instituted only by authorized
personnel. Input to and output from the computer or related system of
formulas or other records or data shall be checked for accuracy. The
degree and frequency of input/output verification shall be based on
the complexity and reliability of the computer or related system. A
backup file of data entered into the computer or related system shall
be maintained except where certain data, such as calculations
performed in connection with laboratory analysis, are eliminated by
computerization or other automated processes. In such instances a
written record of the program shall be maintained along with
appropriate validation data. Hard copy or alternative systems, such as
duplicates, tapes, or microfilm, designed to assure that backup data
are exact and complete and that it is secure from alteration,
inadvertent erasures, or loss shall be maintained.
[43 FR 45077, Sept. 29, 1978, as amended at 60 FR 4091, Jan. 20,
1995]
§ 211.72 Filters.
Filters for liquid filtration used in the manufacture, processing,
or packing of injectable drug products intended for human use shall
not release fibers into such products. Fiber-releasing filters may not
be used in the manufacture, processing, or packing of these injectable
drug products unless it is not possible to manufacture such drug
products without the use of such filters. If use of a fiber-releasing
filter is necessary, an additional non-fiber-releasing filter of 0.22
micron maximum mean porosity (0.45 micron if the manufacturing
conditions so dictate) shall subsequently be used to reduce the
content of particles in the injectable drug product. Use of an
asbestos-containing filter, with or without subsequent use of a
specific non-fiber-releasing filter, is permissible only upon
submission of proof to the appropriate bureau of the Food and Drug
Administration that use of a non-fiber-releasing filter will, or is
likely to, compromise the safety or effectiveness of the injectable
drug product.
Subpart E-Control of Components and
Drug Product Containers and Closures
§ 211.80 General requirements.
(a) There shall be written procedures describing in sufficient
detail the receipt, identification, storage, handling, sampling,
testing, and approval or rejection of components and drug product
containers and closures; such written procedures shall be followed.
(b) Components and drug product containers and closures shall at
all times be handled and stored in a manner to prevent contamination.
(c) Bagged or boxed components of drug product containers, or
closures shall be stored off the floor and suitably spaced to permit
cleaning and inspection.
(d) Each container or grouping of containers for components or drug
product containers, or closures shall be identified with a distinctive
code for each lot in each shipment received. This code shall be used
in recording the disposition of each lot. Each lot shall be
appropriately identified as to its status (i.e., quarantined,
approved, or rejected).
§ 211.82 Receipt and storage of untested
components, drug product containers, and closures.
(a) Upon receipt and before acceptance,
each container or grouping of containers of components, drug product
containers, and closures shall be examined visually for appropriate
labeling as to contents, container damage or broken seals, and
contamination.
(b) Components, drug product containers, and closures shall be
stored under quarantine until they have been tested or examined, as
appropriate, and released. Storage within the area shall conform to
the requirements of §211.80.
§ 211.84 Testing and approval or rejection
of components, drug product containers, and closures.
(a) Each lot of components, drug product containers, and closures
shall be withheld from use until the lot has been sampled, tested, or
examined, as appropriate, and released for use by the quality control
unit.
(b) Representative samples of each shipment of each lot shall be
collected for testing or examination. The number of containers to be
sampled, and the amount of material to be taken from each container,
shall be based upon appropriate criteria such as statistical criteria
for component variability, confidence levels, and degree of precision
desired, the past quality history of the supplier, and the quantity
needed for analysis and reserve where required by § 211.170.
(c) Samples shall be collected in accordance with the following
procedures:
(1) The containers of components selected shall be cleaned where
necessary, by appropriate means.
(2) The containers shall be opened, sampled, and resealed in a
manner designed to prevent contamination of their contents and
contamination of other components, drug product containers, or
closures.
(3) Sterile equipment and aseptic sampling techniques shall be used
when necessary.
(4) If it is necessary to sample a component from the top, middle,
and bottom of its container, such sample subdivisions shall not be
composited for testing.
(5) Sample containers shall be identified so that the following
information can be determined: name of the material sampled, the lot
number, the container from which the sample was taken, the date on
which the sample was taken, and the name of the person who collected
the sample.
(6) Containers from which samples have been taken shall be marked
to show that samples have been removed from them.
(d) Samples shall be examined and tested as
follows:
(1) At least one test shall be conducted to verify the identity of
each component of a drug product. Specific identity tests, if they
exist, shall be used.
(2) Each component shall be tested for conformity with all
appropriate written specifications for purity, strength, and quality.
In lieu of such testing by the manufacturer, a report of analysis may
be accepted from the supplier of a component, provided that at least
one specific identity test is conducted on such component by the
manufacturer, and provided that the manufacturer establishes the
reliability of the supplier's analyses through appropriate validation
of the supplier's test results at appropriate intervals.
(3) Containers and closures shall be tested for conformance with
all appropriate written procedures. In lieu of such testing by the
manufacturer, a certificate of testing may be accepted from the
supplier, provided that at least a visual identification is conducted
on such containers/closures by the manufacturer and provided that the
manufacturer establishes the reliability of the supplier's test
results through appropriate validation of the supplier's test results
at appropriate intervals.
(4) When appropriate, components shall be microscopically examined.
(5) Each lot of a component, drug product container, or closure
that is liable to contamination with filth, insect infestation, or
other extraneous adulterant shall be examined against established
specifications for such contamination.
(6) Each lot of a component, drug product container, or closure
that is liable to microbiological contamination that is objectionable
in view of its intended use shall be subjected to microbiological
tests before use.
(e) Any lot of components, drug product containers, or closures
that meets the appropriate written specifications of identity,
strength, quality, and purity and related tests under paragraph (d) of
this section may be approved and released for use. Any lot of such
material that does not meet such specifications shall be rejected.
§ 211.86 Use of approved components, drug
product containers, and closures.
Components, drug product containers, and closures approved for use
shall be rotated so that the oldest approved stock is used first.
Deviation from this requirement is permitted if such deviation is
temporary and appropriate.
§ 211.87 Retesting of approved components,
drug product containers, and closures.
Components, drug product containers, and closures shall be retested
or reexamined, as appropriate, for identity, strength, quality, and
purity and approved or rejected by the quality control unit in
accordance with § 211.84 as necessary, e.g., after storage for long
periods or after exposure to air, heat or other conditions that might
adversely affect the component, drug product container, or closure.
§ 211.89 Rejected components, drug product
containers, and closures.
Rejected components, drug product containers, and closures shall be
identified and controlled under a quarantine system designed to
prevent their use in manufacturing or processing operations for which
they are unsuitable.
§ 211.94 Drug product containers and
closures.
(a) Drug product containers and closures shall not be reactive,
additive, or absorptive so as to alter the safety, identity, strength,
quality, or purity of the drug beyond the official or established
requirements.
(b) Container closure systems shall provide adequate protection
against foreseeable external factors in storage and use that can cause
deterioration or contamination of the drug product. (c) Drug product
containers and closures shall be clean and, where indicated by the
nature of the drug, sterilized and processed to remove pyrogenic
properties to assure that they are suitable for their intended use.
(d) Standards or specifications, methods of testing, and, where
indicated, methods of cleaning, sterilizing, and processing to remove
pyrogenic properties shall be written and followed for drug product
containers and closures.
Subpart F-Production and Process
Controls
§ 211.100 Written procedures; deviations.
(a) There shall be written procedures for production and process
control designed to assure that the drug products have the identity,
strength, quality, and purity they purport or are represented to
possess. Such procedures shall include all requirements in this
subpart. These written procedures, including any changes, shall be
drafted, reviewed, and approved by the appropriate organizational
units and reviewed and approved by the quality control unit.
(b) Written production and process control procedures shall be
followed in the execution of the various production and process
control functions and shall be documented at the time of performance.
Any deviation from the written procedures shall be recorded and
justified.
§ 211.101 Charge-in of components.
Written production and control procedures shall include the
following, which are designed to assure that the drug products
produced have the identity, strength, quality, and purity they purport
or are represented to possess:
(a) The batch shall be formulated with the intent to provide not
less than 100 percent of the labeled or established amount of active
ingredient.
(b) Components for drug product manufacturing shall be weighed,
measured, or subdivided as appropriate. If a component is removed from
the original container to another, the new container shall be
identified with the following information:
(1) Component name or item code;
(2) Receiving or control number;
(3) Weight or measure in new container;
(4) Batch for which component was dispensed, including its product
name, strength, and lot number.
(c) Weighing, measuring, or subdividing operations for components
shall be adequately supervised. Each container of component dispensed
to manufacturing shall be examined by a second person to assure that:
(1) The component was released by the quality control unit;
(2) The weight or measure is correct as stated in the batch
production records;
(3) The containers are properly identified.
(d) Each component shall be added to the batch by one person and
verified by a second person.
§ 211.103 Calculation of yield.
Actual yields and percentages of theoretical yield shall be
determined at the conclusion of each appropriate phase of
manufacturing, processing, packaging, or holding of the drug product.
Such calculations shall be performed by one person and independently
verified by a second person.
§ 211.105 Equipment identification.
(a) All compounding and storage containers, processing lines, and
major equipment used during the production of a batch of a drug
product shall be properly identified at all times to indicate their
contents and, when necessary, the phase of processing of the batch.
(b) Major equipment shall be identified by a distinctive
identification number or code that shall be recorded in the batch
production record to show the specific equipment used in the
manufacture of each batch of a drug product. In cases where only one
of a particular type of equipment exists in a manufacturing facility,
the name of the equipment may be used in lieu of a distinctive
identification number or code.
§ 211.110 Sampling and testing of
in-process materials and drug products.
(a) To assure batch uniformity and integrity of drug products,
written procedures shall be established and followed that describe the
in-process controls, and tests, or examinations to be conducted on
appropriate samples of in-process materials of each batch. Such
control procedures shall be established to monitor the output and to
validate the performance of those manufacturing processes that may be
responsible for causing variability in the characteristics of
in-process material and the drug product. Such control procedures
shall include, but are not limited to, the following, where
appropriate:
(1) Tablet or capsule weight variation;
(2) Disintegration time;
(3) Adequacy of mixing to assure uniformity and homogeneity;
(4) Dissolution time and rate;
(5) Clarity, completeness, or pH of solutions.
(b) Valid in-process specifications for such characteristics shall
be consistent with drug product final specifications and shall be
derived from previous acceptable process average and process
variability estimates where possible and determined by the application
of suitable statistical procedures where appropriate. Examination and
testing of samples shall assure that the drug product and in-process
material conform to specifications.
(c) In-process materials shall be tested for identity, strength,
quality, and purity as appropriate, and approved or rejected by the
quality control unit, during the production process, e.g., at
commencement or completion of significant phases or after storage for
long periods.
(d) Rejected in-process materials shall be identified and
controlled under a quarantine system designed to prevent their use in
manufacturing or processing operations for which they are unsuitable.
§ 211.111 Time limitations on production.
When appropriate, time limits for the completion of each phase of
production shall be established to assure the quality of the drug
product. Deviation from established time limits may be acceptable if
such deviation does not compromise the quality of the drug product.
Such deviation shall be justified and documented.
§ 211.113 Control of microbiological
contamination.
(a) Appropriate written procedures, designed to prevent
objectionable microorganisms in drug products not required to be
sterile, shall be established and followed.
(b) Appropriate written procedures, designed to prevent
microbiological contamination of drug products purporting to be
sterile, shall be established and followed. Such procedures shall
include validation of any sterilization process.
§ 211.115 Reprocessing.
(a) Written procedures shall be established and followed
prescribing a system for reprocessing batches that do not conform to
standards or specifications and the steps to be taken to insure that
the reprocessed batches will conform with all established standards,
specifications, and characteristics.
(b) Reprocessing shall not be performed without the review and
approval of the quality control unit.
Subpart G-Packaging and Labeling
Control
§ 211.122 Materials examination and usage
criteria.
(a) There shall be written procedures
describing in sufficient detail the receipt, identification, storage,
handling, sampling, examination, and/or testing of labeling and
packaging materials; such written procedures shall be followed.
Labeling and packaging materials shall be representatively sampled,
and examined or tested upon receipt and before use in packaging or
labeling of a drug product.
(b) Any labeling or packaging materials meeting appropriate written
specifications may be approved and released for use. Any labeling or
packaging materials that do not meet such specifications shall be
rejected to prevent their use in operations for which they are
unsuitable.
(c) Records shall be maintained for each
shipment received of each different labeling and packaging material
indicating receipt, examination or testing, and whether accepted or
rejected.
(d) Labels and other labeling materials for each different drug
product, strength, dosage form, or quantity of contents shall be
stored separately with suitable identification. Access to the storage
area shall be limited to authorized personnel.
(e) Obsolete and outdated labels, labeling, and other packaging
materials shall be destroyed.
(f) Use of gang printing of labeling for different drug products or
different strengths or net contents of the same drug product, is
prohibited unless the labeling from gang-printed sheets is adequately
differentiated by size, shape, or color.
(g) If cut labeling is used, packaging and labeling operations
shall include one of the following special control procedures:
(1) Dedication of labeling and packaging lines to each different
strength of each different drug product.
(2) Use of appropriate electronic or
electromechanical equipment to conduct a 100- percent examination for
correct labeling during or after completion of finishing operations;
or
(3) Use of visual inspection to conduct a 100- percent examination
for correct labeling during or after completion of finishing
operations for hand- applied labeling. Such examination shall be
performed by one person and independently verified by a second person.
(h) Printing devices on, or associated with, manufacturing lines
used to imprint labeling upon the drug product unit label or case
shall be monitored to assure that all imprinting conforms to the print
specified in the batch production record.
[43 FR 45077, Sept. 29, 1978, as amended at 58 FR 41353, Aug. 3,
1993]
§ 211.125 Labeling issuance.
(a) Strict control shall be exercised over labeling issued for use
in drug product labeling operations.
(b) Labeling materials issued for a batch shall be carefully
examined for identity and conformity to the labeling specified in the
master or batch production records.
(c) Procedures shall be utilized to reconcile the quantities of
labeling issued, used, and returned, and shall require evaluation of
discrepancies found between the quantity of drug product finished and
the quantity of labeling issued when such discrepancies are outside
narrow preset limits based on historical operating data. Such
discrepancies shall be investigated in accordance with § 211.192.
Labeling reconciliation is waived for cut or roll labeling if a
100-percent examination for correct labeling is performed in
accordance with § 211.122(g)(2).
(d) All excess labeling bearing lot or control numbers shall be
destroyed.
(e) Returned labeling shall be maintained and stored in a manner to
prevent mixups and provide proper identification.
(f) Procedures shall be written describing in sufficient detail the
control procedures employed for the issuance of labeling; such written
procedures shall be followed.
[43 FR 45077, Sept. 29, 1978, as amended at 58 FR 41345, Aug. 3,
1993]
§ 211.130 Packaging and labeling
operations.
There shall be written procedures designed to assure that correct
labels, labeling, and packaging materials are used for drug products;
such written procedures shall be followed. These procedures shall
incorporate the following features:
(a) Prevention of mixups and cross-contamination by physical or
spatial separation from operations on other drug products.
(b) Identification and handling of filled drug product containers
that are set aside and held in unlabeled condition for future labeling
operations to preclude mislabeling of individual containers, lots, or
portions of lots. Identification need not be applied to each
individual container but shall be sufficient to determine name,
strength, quantity of contents, and lot or control number of each
container.
(c) Identification of the drug product
with a lot or control number that permits determination of the history
of the manufacture and control of the batch.
(d) Examination of packaging and labeling materials for suitability
and correctness before packaging operations, and documentation of such
examination in the batch production record.
(e) Inspection of the packaging and labeling facilities immediately
before use to assure that all drug products have been removed from
previous operations. Inspection shall also be made to assure that
packaging and labeling materials not suitable for subsequent
operations have been removed. Results of inspection shall be
documented in the batch production records.
[43 FR 45077, Sept. 29, 1978, as amended at 58 FR 41354, Aug. 3,
1993]
§ 211.132 Tamper-resistant packaging
requirements for over-the-counter (OTC) human drug products.
(a) General. The Food and Drug Administration has the
authority under the Federal Food, Drug, and Cosmetic Act (the act) to
establish a uniform national requirement for tamper-resistant
packaging of OTC drug products that will improve the security of OTC
drug packaging and help assure the safety and effectiveness of OTC
drug products. An OTC drug product (except a dermatological,
dentifrice, insulin, or throat lozenge product) for retail sale that
is not packaged in a tamper-resistant package or that is not properly
labeled under this section is adulterated under section 501 of the act
or misbranded under section 502 of the act, or both.
(b) Requirement for tamper-resistant package. Each
manufacturer and packer who packages an OTC drug product (except a
dermatological, dentifrice, insulin, or throat lozenge product) for
retail sale shall package the product in a tamper-resistant package,
if this product is accessible to the public while held for sale. A
tamper-resistant package is one having one or more indicators or
barriers to entry which, if breached or missing, can reasonably be
expected to provide visible evidence to consumers that tampering has
occurred. To reduce the likelihood of successful tampering and to
increase the likelihood that consumers will discover if a product has
been tampered with, the package is required to be distinctive by
design (e.g., an aerosol product container) or by the use of one or
more indicators or barriers to entry that employ an identifying
characteristic (e.g., a pattern, name, registered trademark, logo, or
picture). For purposes of this section, the term "distinctive by
design'' means the packaging cannot be duplicated with commonly
available materials or through commonly available processes. For
purposes of this section, the term "aerosol product'' means a product
which depends upon the power of a liquified or compressed gas to expel
the contents from the container. A tamper-resistant package may
involve an immediate-container and closure system or secondary-
container or carton system or any combination of systems intended to
provide a visual indication of package integrity. The tamper-
resistant feature shall be designed to and shall remain intact when
handled in a reasonable manner during manufacture, distribution, and
retail display.
(1) For two-piece, hard gelatin capsule products subject to this
requirement, a minimum of two tamper-resistant packaging features is
required, unless the capsules are sealed by a tamper- resistant
technology.
(2) For all other products subject to this requirement, including
two-piece, hard gelatin capsules that are sealed by a tamper-
resistant technology, a minimum of one tamper-resistant feature is
required.
(c) Labeling. Each retail package of an OTC drug product
covered by this section, except ammonia inhalant in crushable glass
ampules, aerosol products as defined in paragraph (b) of this section,
or containers of compressed medical oxygen, is required to bear a
statement that is prominently placed so that consumers are alerted to
the specific tamper-resistant feature of the package. The labeling
statement is also required to be so placed that it will be unaffected
if the tamper-resistant feature of the package is breached or missing.
If the tamper-resistant feature chosen to meet the requirement in
paragraph (b) of this section is one that uses an identifying
characteristic, that characteristic is required to be referred to in
the labeling statement. For example, the labeling statement on a
bottle with a shrink band could say "For your protection, this bottle
has an imprinted seal around the neck.''
(d) Request for exemptions from packaging and labeling
requirements. A manufacturer or packer may request an exemption
from the packaging and labeling requirements of this section. A
request for an exemption is required to be submitted in the form of a
citizen petition under § 10.30 of this chapter and should be clearly
identified on the envelope as a "Request for Exemption from
Tamper-Resistant Rule.'' The petition is required to contain the
following:
(1) The name of the drug product or, if the petition seeks an
exemption for a drug class, the name of the drug class, and a list of
products within that class.
(2) The reasons that the drug product's compliance with the
tamper-resistant packaging or labeling requirements of this section is
unnecessary or cannot be achieved.
(3) A description of alternative steps that are available, or that
the petitioner has already taken, to reduce the likelihood that the
product or drug class will be the subject of malicious adulteration.
(4) Other information justifying an exemption.
(e) OTC drug products subject to approved new drug applications.
Holders of approved new drug applications for OTC drug products
are required under § 314.70 of this chapter to provide the agency with
notification of changes in packaging and labeling to comply with the
requirements of this section. Changes in packaging and labeling
required by this regulation may be made before FDA approval, as
provided under § 314.70(c) of this chapter. Manufacturing changes by
which capsules are to be sealed require prior FDA approval under §
314.70(b) of this chapter.
(f) Poison Prevention Packaging Act of 1970. This section
does not affect any requirements for "special packaging'' as defined
under § 310.3(l) of this chapter and required under the Poison
Prevention Packaging Act of 1970.
(Approved by the Office of Management and Budget under OMB control
number 0910-0149)
[54 FR 5228, Feb. 2, 1989]
§ 211.134 Drug product inspection.
(a) Packaged and labeled products shall be examined during
finishing operations to provide assurance that containers and packages
in the lot have the correct label.
(b) A representative sample of units shall be collected at the
completion of finishing operations and shall be visually examined for
correct labeling.
(c) Results of these examinations shall be recorded in the batch
production or control records.
§ 211.137 Expiration dating.
(a) To assure that a drug product meets applicable standards of
identity, strength, quality, and purity at the time of use, it shall
bear an expiration date determined by appropriate stability testing
described in § 211.166.
(b) Expiration dates shall be related to any storage conditions
stated on the labeling, as determined by stability studies described
in §211.166.
(c) If the drug product is to be reconstituted at the time of
dispensing, its labeling shall bear expiration information for both
the reconstituted and unreconstituted drug products.
(d) Expiration dates shall appear on labeling in accordance with
the requirements of § 201.17 of this chapter.
(e) Homeopathic drug products shall be exempt from the requirements
of this section.
(f) Allergenic extracts that are labeled "No U.S. Standard of
Potency'' are exempt from the requirements of this section.
(g) New drug products for investigational use are exempt from the
requirements of this section, provided that they meet appropriate
standards or specifications as demonstrated by stability studies
during their use in clinical investigations. Where new drug products
for investigational use are to be reconstituted at the time of
dispensing, their labeling shall bear expiration information for the
reconstituted drug product.
(h) Pending consideration of a proposed exemption, published in the
Federal Register of September 29, 1978, the requirements in this
section shall not be enforced for human OTC drug products if their
labeling does not bear dosage limitations and they are stable for at
least 3 years as supported by appropriate stability data.
[43 FR 45077, Sept. 29, 1978, as amended at 46 FR 56412, Nov. 17,
1981; 60 FR 4091, Jan. 20, 1995]
Subpart H-Holding and Distribution
§ 211.142 Warehousing procedures.
Written procedures describing the warehousing of drug products
shall be established and followed. They shall include:
(a) Quarantine of drug products before release by the quality
control unit.
(b) Storage of drug products under appropriate conditions of
temperature, humidity, and light so that the identity, strength,
quality, and purity of the drug products are not affected.
§ 211.150 Distribution procedures.
Written procedures shall be established, and followed, describing
the distribution of drug products. They shall include:
(a) A procedure whereby the oldest approved stock of a drug product
is distributed first. Deviation from this requirement is permitted if
such deviation is temporary and appropriate.
(b) A system by which the distribution of each lot of drug product
can be readily determined to facilitate its recall if necessary.
Subpart I-Laboratory Controls
§ 211.160 General requirements.
(a) The establishment of any specifications, standards, sampling
plans, test procedures, or other laboratory control mechanisms
required by this subpart, including any change in such specifications,
standards, sampling plans, test procedures, or other laboratory
control mechanisms, shall be drafted by the appropriate organizational
unit and reviewed and approved by the quality control unit. The
requirements in this subpart shall be followed and shall be documented
at the time of performance. Any deviation from the written
specifications, standards, sampling plans, test procedures, or other
laboratory control mechanisms shall be recorded and justified.
(b) Laboratory controls shall include the establishment of
scientifically sound and appropriate specifications, standards,
sampling plans, and test procedures designed to assure that
components, drug product containers, closures, in-process materials,
labeling, and drug products conform to appropriate standards of
identity, strength, quality, and purity. Laboratory controls shall
include:
(1) Determination of conformance to appropriate written
specifications for the acceptance of each lot within each shipment of
components, drug product containers, closures, and labeling used in
the manufacture, processing, packing, or holding of drug products. The
specifications shall include a description of the sampling and testing
procedures used. Samples shall be representative and adequately
identified. Such procedures shall also require appropriate retesting
of any component, drug product container, or closure that is subject
to deterioration.
(2) Determination of conformance to written specifications and a
description of sampling and testing procedures for in-process
materials. Such samples shall be representative and properly
identified.
(3) Determination of conformance to written descriptions of
sampling procedures and appropriate specifications for drug products.
Such samples shall be representative and properly identified.
(4) The calibration of instruments,
apparatus, gauges, and recording devices at suitable intervals in
accordance with an established written program containing specific
directions, schedules, limits for accuracy and precision, and
provisions for remedial action in the event accuracy and/or precision
limits are not met. Instruments, apparatus, gauges, and recording
devices not meeting established specifications shall not be used.
§ 211.165 Testing and release for
distribution.
(a) For each batch of drug product, there shall be appropriate
laboratory determination of satisfactory conformance to final
specifications for the drug product, including the identity and
strength of each active ingredient, prior to release. Where sterility
and/or pyrogen testing are conducted on specific batches of shortlived
radiopharmaceuticals, such batches may be released prior to completion
of sterility and/or pyrogen testing, provided such testing is
completed as soon as possible.
(b) There shall be appropriate laboratory testing, as necessary, of
each batch of drug product required to be free of objectionable
microorganisms.
(c) Any sampling and testing plans shall be described in written
procedures that shall include the method of sampling and the number of
units per batch to be tested; such written procedure shall be
followed.
(d) Acceptance criteria for the sampling and testing conducted by
the quality control unit shall be adequate to assure that batches of
drug products meet each appropriate specification and appropriate
statistical quality control criteria as a condition for their approval
and release. The statistical quality control criteria shall include
appropriate acceptance levels and/or appropriate rejection levels.
(e) The accuracy, sensitivity, specificity, and reproducibility of
test methods employed by the firm shall be established and documented.
Such validation and documentation may be accomplished in accordance
with § 211.194(a)(2).
(f) Drug products failing to meet established standards or
specifications and any other relevant quality control criteria shall
be rejected. Reprocessing may be performed. Prior to acceptance and
use, reprocessed material must meet appropriate standards,
specifications, and any other relevant criteria.
§ 211.166 Stability testing.
(a) There shall be a written testing program designed to assess the
stability characteristics of drug products. The results of such
stability testing shall be used in determining appropriate storage
conditions and expiration dates. The written program shall be followed
and shall include:
(1) Sample size and test intervals based on statistical criteria
for each attribute examined to assure valid estimates of stability;
(2) Storage conditions for samples retained for testing;
(3) Reliable, meaningful, and specific test methods;
(4) Testing of the drug product in the same container-closure
system as that in which the drug product is marketed;
(5) Testing of drug products for reconstitution at the time of
dispensing (as directed in the labeling) as well as after they are
reconstituted.
(b) An adequate number of batches of each drug product shall be
tested to determine an appropriate expiration date and a record of
such data shall be maintained. Accelerated studies, combined with
basic stability information on the components, drug products, and
container-closure system, may be used to support tentative expiration
dates provided full shelf life studies are not available and are being
conducted. Where data from accelerated studies are used to project a
tentative expiration date that is beyond a date supported by actual
shelf life studies, there must be stability studies conducted,
including drug product testing at appropriate intervals, until the
tentative expiration date is verified or the appropriate expiration
date determined.
(c) For homeopathic drug products, the requirements of this section
are as follows:
(1) There shall be a written assessment of stability based at least
on testing or examination of the drug product for compatibility of the
ingredients, and based on marketing experience with the drug product
to indicate that there is no degradation of the product for the normal
or expected period of use.
(2) Evaluation of stability shall be based on the same
container-closure system in which the drug product is being marketed.
(d) Allergenic extracts that are labeled "No U.S. Standard of
Potency'' are exempt from the requirements of this section.
[43 FR 45077, Sept. 29, 1978, as amended at 46 FR 56412, Nov. 17,
1981]
§ 211.167 Special testing requirements.
(a) For each batch of drug product purporting to be sterile and/or
pyrogen-free, there shall be appropriate laboratory testing to
determine conformance to such requirements. The test procedures shall
be in writing and shall be followed.
(b) For each batch of ophthalmic ointment, there shall be
appropriate testing to determine conformance to specifications
regarding the presence of foreign particles and harsh or abrasive
substances. The test procedures shall be in writing and shall be
followed.
(c) For each batch of controlled-release dosage form, there shall
be appropriate laboratory testing to determine conformance to the
specifications for the rate of release of each active ingredient. The
test procedures shall be in writing and shall be followed.
§ 211.170 Reserve samples.
(a) An appropriately identified reserve sample that is
representative of each lot in each shipment of each active ingredient
shall be retained. The reserve sample consists of at least twice the
quantity necessary for all tests required to determine whether the
active ingredient meets its established specifications, except for
sterility and pyrogen testing. The retention time is as follows:
(1) For an active ingredient in a drug product other than those
described in paragraphs (a) (2) and (3) of this section, the reserve
sample shall be retained for 1 year after the expiration date of the
last lot of the drug product containing the active ingredient.
(2) For an active ingredient in a radioactive drug product, except
for nonradioactive reagent kits, the reserve sample shall be retained
for:
(I) Three months after the expiration date of the last lot of the
drug product containing the active ingredient if the expiration dating
period of the drug product is 30 days or less; or
(ii) Six months after the expiration date of the last lot of the
drug product containing the active ingredient if the expiration dating
period of the drug product is more than 30 days.
(3) For an active ingredient in an OTC drug product that is exempt
from bearing an expiration date under § 211.137, the reserve sample
shall be retained for 3 years after distribution of the last lot of
the drug product containing the active ingredient.
(b) An appropriately identified reserve sample that is
representative of each lot or batch of drug product shall be retained
and stored under conditions consistent with product labeling. The
reserve sample shall be stored in the same immediate container-closure
system in which the drug product is marketed or in one that has
essentially the same characteristics. The reserve sample consists of
at least twice the quantity necessary to perform all the required
tests, except those for sterility and pyrogens. Except for those drug
products described in paragraph (b)(2) of this section, reserve
samples from representative sample lots or batches selected by
acceptable statistical procedures shall be examined visually at least
once a year for evidence of deterioration unless visual examination
would affect the integrity of the reserve sample. Any evidence of
reserve sample deterioration shall be investigated in accordance with
§ 211.192. The results of examination shall be recorded and maintained
with other stability data on the drug product. Reserve samples of
compressed medical gases need not be retained. The retention time is
as follows:
(1) For a drug product other than those described in paragraphs (b)
(2) and (3) of this section, the reserve sample shall be retained for
1 year after the expiration date of the drug product.
(2) For a radioactive drug product, except for nonradioactive
reagent kits, the reserve sample shall be retained for:
(I) Three months after the expiration date of the drug product if
the expiration dating period of the drug product is 30 days or less;
or
(ii) Six months after the expiration date of the drug product if
the expiration dating period of the drug product is more than 30 days.
(3) For an OTC drug product that is exempt for bearing an
expiration date under § 211.137, the reserve sample must be retained
for 3 years after the lot or batch of drug product is distributed.
[48 FR 13025, Mar. 29, 1983, as amended at 60 FR 4091, Jan. 20,
1995]
§ 211.173 Laboratory animals.
Animals used in testing components, in-process materials, or drug
products for compliance with established specifications shall be
maintained and controlled in a manner that assures their suitability
for their intended use. They shall be identified, and adequate records
shall be maintained showing the history of their use.
§ 211.176 Penicillin contamination.
If a reasonable possibility exists that a non-penicillin drug
product has been exposed to cross-contamination with penicillin, the
non-penicillin drug product shall be tested for the presence of
penicillin. Such drug product shall not be marketed if detectable
levels are found when tested according to procedures specified in
`Procedures for Detecting and Measuring Penicillin Contamination in
Drugs,' which is incorporated by reference. Copies are available from
the Division of Research and Testing (HFD-470), Center for Drug
Evaluation and Research, Food and Drug Administration, 200 C St. SW.,
Washington, DC 20204, or available for inspection at the Office of the
Federal Register, 800 North Capitol Street, NW., suite 700,
Washington, DC 20408.
[43 FR 45077, Sept. 29, 1978, as amended at 47 FR 9396, Mar. 5,
1982; 50 FR 8996, Mar. 6, 1985; 55 FR 11577, Mar. 29, 1990]
Subpart J-Records and Reports
§ 211.180 General requirements.
(a) Any production, control, or distribution record that is
required to be maintained in compliance with this part and is
specifically associated with a batch of a drug product shall be
retained for at least 1 year after the expiration date of the batch
or, in the case of certain OTC drug products lacking expiration dating
because they meet the criteria for exemption under § 211.137, 3 years
after distribution of the batch.
(b) Records shall be maintained for all components, drug product
containers, closures, and labeling for at least 1 year after the
expiration date or, in the case of certain OTC drug products lacking
expiration dating because they meet the criteria for exemption under §
211.137, 3 years after distribution of the last lot of drug product
incorporating the component or using the container, closure, or
labeling.
(c) All records required under this part,
or copies of such records, shall be readily available for authorized
inspection during the retention period at the establishment where the
activities described in such records occurred. These records or copies
thereof shall be subject to photocopying or other means of
reproduction as part of such inspection. Records that can be
immediately retrieved from another location by computer or other
electronic means shall be considered as meeting the requirements of
this paragraph.
(d) Records required under this part may be retained either as
original records or as true copies such as photocopies, microfilm,
microfiche, or other accurate reproductions of the original records.
Where reduction techniques, such as microfilming, are used, suitable
reader and photocopying equipment shall be readily available.
(e) Written records required by this part shall be maintained so
that data therein can be used for evaluating, at least annually, the
quality standards of each drug product to determine the need for
changes in drug product specifications or manufacturing or control
procedures. Written procedures shall be established and followed for
such evaluations and shall include provisions for:
(1) A review of a representative number of batches, whether
approved or rejected, and, where applicable, records associated with
the batch.
(2) A review of complaints, recalls, returned or salvaged drug
products, and investigations conducted under § 211.192 for each drug
product.
(f) Procedures shall be established to assure that the responsible
officials of the firm, if they are not personally involved in or
immediately aware of such actions, are notified in writing of any
investigations conducted under §§ 211.198, 211.204, or 211.208 of
these regulations, any recalls, reports of inspectional observations
issued by the Food and Drug Administration, or any regulatory actions
relating to good manufacturing practices brought by the Food and Drug
Administration.
[43 FR 45077, Sept. 29, 1978, as amended at 60 FR 4901, Jan. 20,
1995]
§ 211.182 Equipment cleaning and use log.
A written record of major equipment cleaning, maintenance (except
routine maintenance such as lubrication and adjustments), and use
shall be included in individual equipment logs that show the date,
time, product, and lot number of each batch processed. If equipment is
dedicated to manufacture of one product, then individual equipment
logs are not required, provided that lots or batches of such product
follow in numerical order and are manufactured in numerical sequence.
In cases where dedicated equipment is employed, the records of
cleaning, maintenance, and use shall be part of the batch record. The
persons performing and double-checking the cleaning and maintenance
shall date and sign or initial the log indicating that the work was
performed. Entries in the log shall be in chronological order.
§ 211.184 Component, drug product
container, closure, and labeling records.
These records shall include the following:
(a) The identity and quantity of each shipment of each lot of
components, drug product containers, closures, and labeling; the name
of the supplier; the supplier's lot number(s) if known; the receiving
code as specified in § 211.80; and the date of receipt. The name and
location of the prime manufacturer, if different from the supplier,
shall be listed if known.
(b) The results of any test or examination performed (including
those performed as required by § 211.82(a), § 211.84(d), or
§211.122(a)) and the conclusions derived there from.
(c) An individual inventory record of each component, drug product
container, and closure and, for each component, a reconciliation of
the use of each lot of such component. The inventory record shall
contain sufficient information to allow determination of any batch or
lot of drug product associated with the use of each component, drug
product container, and closure.
(d) Documentation of the examination and review of labels and
labeling for conformity with established specifications in accord with
§§ 211.122(c) and 211.130(c).
(e) The disposition of rejected components, drug product
containers, closure, and labeling.
§ 211.186 Master production and control
records.
(a) To assure uniformity from batch to batch, master production and
control records for each drug product, including each batch size
thereof, shall be prepared, dated, and signed (full signature,
handwritten) by one person and independently checked, dated, and
signed by a second person. The preparation of master production and
control records shall be described in a written procedure and such
written procedure shall be followed.
(b) Master production and control records shall include:
(1) The name and strength of the product and a description of the
dosage form;
(2) The name and weight or measure of each active ingredient per
dosage unit or per unit of weight or measure of the drug product, and
a statement of the total weight or measure of any dosage unit;
(3) A complete list of components designated by names or codes
sufficiently specific to indicate any special quality characteristic;
(4) An accurate statement of the weight or measure of each
component, using the same weight system (metric, avoirdupois, or
apothecary) for each component. Reasonable variations may be
permitted, however, in the amount of components necessary for the
preparation in the dosage form, provided they are justified in the
master production and control records;
(5) A statement concerning any calculated excess of component;
(6) A statement of theoretical weight or measure at appropriate
phases of processing;
(7) A statement of theoretical yield, including the maximum and
minimum percentages of theoretical yield beyond which investigation
according to § 211.192 is required;
(8) A description of the drug product containers, closures, and
packaging materials, including a specimen or copy of each label and
all other labeling signed and dated by the person or persons
responsible for approval of such labeling;
(9) Complete manufacturing and control instructions, sampling and
testing procedures, specifications, special notations, and precautions
to be followed.
§ 211.188 Batch production and control
records.
Batch production and control records shall be prepared for each
batch of drug product produced and shall include complete information
relating to the production and control of each batch. These records
shall include:
(a) An accurate reproduction of the appropriate master production
or control record, checked for accuracy, dated, and signed;
(b) Documentation that each significant step in the manufacture,
processing, packing, or holding of the batch was accomplished,
including:
(1) Dates;
(2) Identity of individual major equipment and lines used;
(3) Specific identification of each batch of component or
in-process material used;
(4) Weights and measures of components used in the course of
processing;
(5) In-process and laboratory control results;
(6) Inspection of the packaging and labeling area before and after
use;
(7) A statement of the actual yield and a statement of the
percentage of theoretical yield at appropriate phases of processing;
(8) Complete labeling control records, including specimens or
copies of all labeling used;
(9) Description of drug product containers and closures;
(10) Any sampling performed;
(11) Identification of the persons performing and directly
supervising or checking each significant step in the operation;
(12) Any investigation made according to § 211.192.
(13) Results of examinations made in accordance with § 211.134.
§ 211.192 Production record review.
All drug product production and control records, including those
for packaging and labeling, shall be reviewed and approved by the
quality control unit to determine compliance with all established,
approved written procedures before a batch is released or distributed.
Any unexplained discrepancy (including a percentage of theoretical
yield exceeding the maximum or minimum percentages established in
master production and control records) or the failure of a batch or
any of its components to meet any of its specifications shall be
thoroughly investigated, whether or not the batch has already been
distributed. The investigation shall extend to other batches of the
same drug product and other drug products that may have been
associated with the specific failure or discrepancy. A written record
of the investigation shall be made and shall include the conclusions
and follow-up.
§ 211.194 Laboratory records.
(a) Laboratory records shall include complete data derived from all
tests necessary to assure compliance with established specifications
and standards, including examinations and assays, as follows:
(1) A description of the sample received for testing with
identification of source (that is, location from where sample was
obtained), quantity, lot number or other distinctive code, date sample
was taken, and date sample was received for testing.
(2) A statement of each method used in the testing of the sample.
The statement shall indicate the location of data that establish that
the methods used in the testing of the sample meet proper standards of
accuracy and reliability as applied to the product tested. (If the
method employed is in the current revision of the United States
Pharmacopeias, National Formulary, Association of Official Analytical
Chemists, Book of Methods,{2} or in other recognized standard
references, or is detailed in an approved new drug application and the
referenced method is not modified, a statement indicating the method
and reference will suffice). The suitability of all testing methods
used shall be verified under actual conditions of use.
{2} Copies may be obtained from: Association of Official Analytical
Chemists, 2200 Wilson Blvd., Suite 400, Arlington, VA 22201-3301.
(3) A statement of the weight or measure of sample used for each
test, where appropriate.
(4) A complete record of all data secured in the course of each
test, including all graphs, charts, and spectra from laboratory
instrumentation, properly identified to show the specific component,
drug product container, closure, in-process material, or drug product,
and lot tested.
(5) A record of all calculations performed in connection with the
test, including units of measure, conversion factors, and equivalency
factors.
(6) A statement of the results of tests and how the results compare
with established standards of identity, strength, quality, and purity
for the component, drug product container, closure, in-process
material, or drug product tested.
(7) The initials or signature of the person who performs each test
and the date's) the tests were performed.
(8) The initials or signature of a second person showing that the
original records have been reviewed for accuracy, completeness, and
compliance with established standards.
(b) Complete records shall be maintained of any modification of an
established method employed in testing. Such records shall include the
reason for the modification and data to verify that the modification
produced results that are at least as accurate and reliable for the
material being tested as the established method.
(c) Complete records shall be maintained of any testing and
standardization of laboratory reference standards, reagents, and
standard solutions.
(d) Complete records shall be maintained of the periodic
calibration of laboratory instruments, apparatus, gauges, and
recording devices required by § 211.160(b)(4).
(e) Complete records shall be maintained of all stability testing
performed in accordance with § 211.166.
[43 FR 45077, Sept. 29, 1978, as amended at 55 FR 11577, Mar. 29,
1990]
§ 211.196 Distribution records.
Distribution records shall contain the name and strength of the
product and description of the dosage form, name and address of the
consignee, date and quantity shipped, and lot or control number of the
drug product. For compressed medical gas products, distribution
records are not required to contain lot or control numbers.
(Approved by the Office of Management and Budget under control
number 0910-0139)
[49 FR 9865, Mar. 16, 1984]
§ 211.198 Complaint files.
(a) Written procedures describing the handling of all written and
oral complaints regarding a drug product shall be established and
followed. Such procedures shall include provisions for review by the
quality control unit, of any complaint involving the possible failure
of a drug product to meet any of its specifications and, for such drug
products, a determination as to the need for an investigation in
accordance with § 211.192. Such procedures shall include provisions
for review to determine whether the complaint represents a serious and
unexpected adverse drug experience which is required to be reported to
the Food and Drug Administration in accordance with § 310.305 of this
chapter.
(b) A written record of each complaint shall be maintained in a
file designated for drug product complaints. The file regarding such
drug product complaints shall be maintained at the establishment where
the drug product involved was manufactured, processed, or packed, or
such file may be maintained at another facility if the written records
in such files are readily available for inspection at that other
facility. Written records involving a drug product shall be maintained
until at least 1 year after the expiration date of the drug product,
or 1 year after the date that the complaint was received, whichever is
longer. In the case of certain OTC drug products lacking expiration
dating because they meet the criteria for exemption under § 211.137,
such written records shall be maintained for 3 years after
distribution of the drug product.
(1) The written record shall include the following information,
where known: the name and strength of the drug product, lot number,
name of complainant, nature of complaint, and reply to complainant.
(2) Where an investigation under § 211.192 is conducted, the
written record shall include the findings of the investigation and
follow up. The record or copy of the record of the investigation shall
be maintained at the establishment where the investigation occurred in
accordance with § 211.180(c).
(3) Where an investigation under § 211.192 is not conducted, the
written record shall include the reason that an investigation was
found not to be necessary and the name of the responsible person
making such a determination.
[43 FR 45077, Sept. 29, 1978, as amended at 51 FR 24479, July 3,
1986]
Subpart K-Returned and Salvaged Drug
Products
§ 211.204 Returned drug products.
Returned drug products shall be identified as such and held. If the
conditions under which returned drug products have been held, stored,
or shipped before or during their return, or if the condition of the
drug product, its container, carton, or labeling, as a result of
storage or shipping, casts doubt on the safety, identity, strength,
quality or purity of the drug product, the returned drug product shall
be destroyed unless examination, testing, or other investigations
prove the drug product meets appropriate standards of safety,
identity, strength, quality, or purity. A drug product may be
reprocessed provided the subsequent drug product meets appropriate
standards, specifications, and characteristics. Records of returned
drug products shall be maintained and shall include the name and label
potency of the drug product dosage form, lot number (or control number
or batch number), reason for the return, quantity returned, date of
disposition, and ultimate disposition of the returned drug product. If
the reason for a drug product being returned implicates associated
batches, an appropriate investigation shall be conducted in accordance
with the requirements of § 211.192. Procedures for the holding,
testing, and reprocessing of returned drug products shall be in
writing and shall be followed.
§ 211.208 Drug product salvaging.
Drug products that have been subjected to improper storage
conditions including extremes in temperature, humidity, smoke, fumes,
pressure, age, or radiation due to natural disasters, fires,
accidents, or equipment failures shall not be salvaged and returned to
the marketplace. Whenever there is a question whether drug products
have been subjected to such conditions, salvaging operations may be
conducted only if there is (a) evidence from laboratory tests and
assays (including animal feeding studies where applicable) that the
drug products meet all applicable standards of identity, strength,
quality, and purity and (b) evidence from inspection of the premises
that the drug products and their associated packaging were not
subjected to improper storage conditions as a result of the disaster
or accident. Organoleptic examinations shall be acceptable only as
supplemental evidence that the drug products meet appropriate
standards of identity, strength, quality, and purity. Records
including name, lot number, and disposition shall be maintained for
drug products subject to this section.
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Date created: August 29, 1996 ; last updated: December 6, 2005
Provided by the US FDA
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