I. INTRODUCTION
This article is written to guide and design how
to set up validation procedure, one must recognize that for cleaning
validation, as with validation of other processes, there may be more than one
way to validate a process. In the end, the test of any validation process is
whether scientific data shows that the system consistently does as expected and
produces a result that consistently meets predetermined specifications.This guide is intended to cover equipment cleaning for chemical residues
only.
II. BACKGROUND
As per FDA require, equipment should be clean
prior to use, the 1963 GMP Regulations (Part 133.4) stated as follows
"Equipment *** shall be maintained in a clean and orderly manner
***." A very similar section on equipment cleaning (211.67) was included
in the 1978 CGMP regulations. Of course, the main rationale for requiring clean
equipment is to prevent contamination or
adulteration of drug products.
Historically, FDA investigators have looked for
gross insanitation due to inadequate cleaning and maintenance of equipment
and/or poor dust control systems. Also, historically speaking, FDA was more
concerned about the contamination of non-penicillin drug products with
penicillins or the cross-contamination of drug products with potent steroids or
hormones. A number of products have been recalled over the past decade due to
actual or potential penicillin cross-contamination.
One event which increased FDA awareness of the potential for cross contamination due to inadequate procedures was the 1988 recall of a finished drug product, Cholestyramine Resin USP. The bulk pharmaceutical chemical used to produce the product had become contaminated with low levels of intermediates and degradants from the production of agricultural pesticides. The cross-contamination in that case is believed to have been due to the reuse of recovered solvents. The recovered solvents had been contaminated because of a lack of control over the reuse of solvent drums. Drums that had been used to store recovered solvents from a pesticide production process were later used to store recovered solvents used for the resin manufacturing process. The firm did not have adequate controls over these solvent drums, did not do adequate testing of drummed solvents, and did not have validated cleaning procedures for the drums.
One event which increased FDA awareness of the potential for cross contamination due to inadequate procedures was the 1988 recall of a finished drug product, Cholestyramine Resin USP. The bulk pharmaceutical chemical used to produce the product had become contaminated with low levels of intermediates and degradants from the production of agricultural pesticides. The cross-contamination in that case is believed to have been due to the reuse of recovered solvents. The recovered solvents had been contaminated because of a lack of control over the reuse of solvent drums. Drums that had been used to store recovered solvents from a pesticide production process were later used to store recovered solvents used for the resin manufacturing process. The firm did not have adequate controls over these solvent drums, did not do adequate testing of drummed solvents, and did not have validated cleaning procedures for the drums.
Some shipments of this pesticide contaminated
bulk pharmaceutical were supplied to a second facility at a different location
for finishing. This resulted in the contamination of the bags used in that
facility's fluid bed dryers with pesticide contamination. This in turn led to
cross contamination of lots produced at that site, a site where no pesticides
were normally produced.
FDA instituted an import alert in 1992 on a
foreign bulk pharmaceutical manufacturer which manufactured potent steroid products as well as non-steroidal
products using common equipment. This firm was a multi-use bulk
pharmaceutical facility. FDA considered the potential for cross-contamination
to be significant and to pose a serious health risk to the public. The firm had
only recently started a cleaning validation program at the time of the
inspection and it was considered inadequate by FDA. One of the reasons it was
considered inadequate was that the firm was only looking for evidence of the
absence of the previous compound. The firm had evidence, from TLC tests on the
rinse water, of the presence of residues of reaction byproducts and degradants
from the previous process.
III. GENERAL REQUIREMENTS
FDA expects firms to have written procedures (SOP's) detailing the cleaning processes used for various pieces of equipment. If firms have one cleaning process for cleaning between different batches of the same product and use a different process for cleaning between product changes, FDA expect that in the written procedures firms should be address both this different scenario. Similarly, if firms have one process for removing water soluble residues and another process for non-water soluble residues, the written procedure should address both scenarios and make it clear when a given procedure is to be followed.
Bulk pharmaceutical firms may decide to dedicate
certain equipment for certain chemical manufacturing process steps that produce
tarry or gummy residues that are difficult to remove from the equipment. Fluid bed dryer bags are another
example of equipment that is difficult to clean and is often dedicated to a
specific product. Any residues from the cleaning process itself (detergents,
solvents, etc.) also have to be removed from the equipment.
FDA expects firms to have written general
procedures on how cleaning processes
will be validated.
FDA expects the general validation procedures
to address who is responsible for
performing and approving the validation study, the acceptance criteria, and
when revalidation will be required.
FDA expects firms to prepare specific written validation protocols in advance
for the studies to be performed on each manufacturing system or piece of
equipment which should address such issues as sampling procedures, and analytical methods to be used including
the sensitivity of those methods.
FDA expects firms to conduct the validation studies in accordance with the protocols and
to document the results of studies.
FDA expects a final
validation report which is approved by management and which states whether
or not the cleaning process is valid.
The data should support a conclusion that residues have been reduced to an "acceptable level."
IV. EVALUATION OF CLEANING VALIDATION
The first step is to focus on the objective of the validation process, and it has been seen that some companies have failed to develop such objectives. It is not unusual to see manufacturers use extensive sampling and testing programs following the cleaning process without ever really evaluating the effectiveness of the steps used to clean the equipment.
Several questions need to be addressed when
evaluating the cleaning process. For example,
What point does a piece of
equipment or system become clean?
Does it have to be scrubbed by
hand?
What is accomplished by hand
scrubbing rather than just a solvent wash?
How variable are manual cleaning
processes from batch to batch and product to product?
The answers to these questions are obviously
important to the inspection and evaluation of the cleaning process since one
must determine the overall effectiveness of the process. Answers to these
questions may also identify steps that can be eliminated for more effective
measures and result in resource savings for the company.
Determine the number of cleaning processes for each
piece of equipment. Ideally, a piece of equipment or system will have one
process for cleaning, however this will depend on the products being produced
and whether the cleanup occurs between batches of the same product (as in a
large campaign) or between batches of different products. When the cleaning
process is used only between batches of the same product (or different lots of
the same intermediate in a bulk process) the firm need only meet a criteria of,
"visibly clean" for the equipment. Such between batch cleaning
processes do not require validation.
1. Equipment Design
Examine the design of equipment, particularly in those large systems that may employ semi-automatic or fully automatic clean-in-place (CIP) systems since they represent significant concern. For example, sanitary type piping without ball valves should be used. When such nonsanitary ball valves are used, as is common in the bulk drug industry, the cleaning process is more difficult.
When such systems are identified, it is
important that operators performing cleaning operations be aware of problems
and has special training in cleaning these systems and valves. Determine
whether the cleaning operators have
knowledge of these systems and the level of training and experience in cleaning
these systems. Also check the written and validated cleaning process to
determine if these systems have been properly identified and validated.
In larger systems, such as those employing long transfer lines or piping, check the flow charts and piping diagrams
for the identification of valves and written cleaning procedures. Piping and valves should be tagged and
easily identifiable by the operator performing the cleaning function.
Sometimes, inadequately identified valves, both on prints and physically, have
led to incorrect cleaning practices.
Always check for the presence of an often critical
element in the documentation of the cleaning processes; identifying and controlling the length of time between the end of
processing and each cleaning step. This is especially important for
topicals, suspensions, and bulk drug operations. In such operations, the drying
of residues will directly affect the efficiency of a cleaning process.
Whether or not
CIP systems are used for cleaning of processing equipment, microbiological
aspects of equipment cleaning should be considered. This consists largely of
preventive measures rather than removal of contamination once it has occurred.
There should be some evidence that
routine cleaning and storage of equipment does not allow microbial
proliferation. For example, equipment
should be dried before storage, and under no circumstances should stagnant
water be allowed to remain in equipment subsequent to cleaning operations.
Subsequent to the cleaning process, equipment may
be subjected to sterilization or
sanitization procedures where such equipment is used for sterile processing, or for nonsterile processing where
the products may support microbial growth. While such sterilization or
sanitization procedures are beyond the scope of this guide, it is important to
note that control of the bioburden
through adequate cleaning and storage of equipment is important to ensure
that subsequent sterilization or
sanitization procedures achieve the necessary assurance of sterility.
This is also particularly important from the
standpoint of the control of pyrogens
in sterile processing since equipment sterilization processes may not be
adequate to achieve significant inactivation or removal of pyrogens.
2. Cleaning
Process Written
Procedure and Documentation
Examine the detail and specificity of the procedure
for the (cleaning) process being validated, and the amount of documentation
required. General SOPs, batch record or
log sheet system that to specific documentation for performing each step.
Depending upon the complexity of the system and
cleaning process and the ability and training of operators, the amount of documentation necessary for executing
various cleaning steps or procedures will vary.
When more complex cleaning procedures are
required, it is important to document the critical
cleaning steps (for example certain bulk drug synthesis processes). In this
regard, specific documentation on the equipment itself which includes information
about who cleaned it and when is
valuable. However, for relatively simple cleaning operations, the mere
documentation that the overall cleaning process was performed might be
sufficient.
Other factors such as history of cleaning, residue levels found after cleaning, and
variability of test results may also dictate the amount of documentation
required. For example, when variable residue levels are detected following
cleaning, particularly for a process that is believed to be acceptable, one
must establish the effectiveness of the process and operator performance.
Appropriate evaluations must be made and when operator performance is deemed a
problem, more extensive documentation (guidance) and training may be required.
3. Analytical Methods
Determine the specificity and sensitivity of the analytical method used to detect residuals or contaminants. With advances in analytical technology, residues from the manufacturing and cleaning processes can be detected at very low levels. If levels of contamination or residual are not detected, it does not mean that there is no residual contaminant present after cleaning. It only means that levels of contaminant greater than the sensitivity or detection limit of the analytical method are not present in the sample. The firm should challenge the analytical method in combination with the sampling method(s) used to show that contaminants can be recovered from the equipment surface and at what level, i.e. 50% recovery, 90%, etc. This is necessary before any conclusions can be made based on the sample results. A negative test may also be the result of poor sampling technique (see below).
4. Sampling
There are two general types of sampling that have been found acceptable. The most desirable is the direct method of sampling the surface of the equipment. Another method is the use of rinse solutions.
a. Direct Surface Sampling - Determine the
type of sampling material used and its impact on the test data since the
sampling material may interfere with the test. For example, the adhesive used in swabs has been found
to interfere with the analysis of samples. Therefore, early in the
validation program, it is important to assure that the sampling medium and solvent (used for extraction from the medium)
are satisfactory and can be readily used.
Advantages of direct sampling are that areas
hardest to clean and which are reasonably accessible can be evaluated, leading
to establishing a level of contamination or residue per given surface area.
Additionally, residues that are "dried out" or are insoluble can be
sampled by physical removal.
b. Rinse Samples - Two advantages of
using rinse samples are that a larger
surface area may be sampled and inaccessible
systems or ones that cannot be routinely disassembled can be sampled and
evaluated.
A disadvantage of rinse samples is that the residue
or contaminant may not be soluble or may be physically may not reach the all
critical location in the equipment.
Check to see that a direct measurement of the
residue or contaminant has been made for the rinse water when it is used to
validate the cleaning process. For example, it is not acceptable to simply test
rinse water for water quality (does it meet the compendia tests) rather than
test it for potential contaminates.
c. Routine Production In-Process Control
Monitoring - Indirect testing, such as conductivity testing, may be of some
value for routine monitoring once a cleaning process has been validated. This
would be particularly true for the bulk drug substance manufacturer where
reactors and centrifuges and piping between such large equipment can be sampled
only using rinse solution samples. Any indirect test method must have been
shown to correlate with the condition of the equipment. During validation, the
firm should document that testing the uncleaned equipment gives a not
acceptable result for the indirect test.
V. ESTABLISHMENT OF LIMITS
FDA does not intend to set acceptance
specifications or methods for determining whether a cleaning process is
validated. It is impractical for FDA to do so due to the wide variation in equipment and products used throughout the bulk and
finished dosage form industries. The firm's rationale for the residue
limits established should be logical based on the manufacturer's knowledge of
the materials involved and be practical, achievable, and verifiable. It is
important to define the sensitivity of
the analytical methods in order to set reasonable limits. Some limits that
have been mentioned by industry representatives in the literature or in
presentations include analytical
detection levels such as 10 PPM, biological activity levels such as 1/1000 of
the normal therapeutic dose, and organoleptic levels such as no visible
residue.
Check the manner in which limits are established.
Unlike finished pharmaceuticals where the chemical identity of residuals are
known (i.e., from actives, inactives, detergents) bulk processes may have
partial reactants and unwanted by-products which may never have been chemically
identified. In establishing residual limits, it may not be adequate to focus
only on the principal reactant since
other chemical variations may be more
difficult to remove. There are circumstances where TLC screening, in
addition to chemical analyses, may be needed. In a bulk process, particularly
for very potent chemicals such as some steroids, the issue of by-products needs
to be considered if equipment is not dedicated. The objective of the inspection
is to ensure that the basis for any limits is scientifically justifiable.
VI. OTHER ISSUES
a. Placebo Product
In order to evaluate and validate cleaning
processes some manufacturers have processed
a placebo batch in the equipment under essentially the same operating
parameters used for processing product. A sample of the placebo batch is then
tested for residual contamination. However, we have documented several significant issues that need to be addressed
when using placebo product to validate
cleaning processes.
One cannot assure that the contaminate will be
uniformly distributed throughout the system. For example, if the discharge
valve or chute of a blender is contaminated, the contaminant would probably not
be uniformly dispersed in the placebo; it would most likely be concentrated in
the initial discharge portion of the batch. Additionally, if the contaminant or residue is of a larger
particle size, it may not be uniformly dispersed in the placebo.
Some firms have made the assumption that a
residual contaminant would be worn off the equipment surface uniformly; this is
also an invalid conclusion. Finally, the analytical power may be greatly
reduced by dilution of the contaminate. Because of such problems, rinse and/or
swab samples should be used in conjunction with the placebo method.
b. Detergent
If a detergent or soap is used for cleaning, determine and consider the difficulty that may arise when attempting to test for residues. A common problem associated with detergent use is its composition. Many detergent suppliers will not provide specific composition, which makes it difficult for the user to evaluate residues. As with product residues, it is important and it is expected that the manufacturer evaluate the efficiency of the cleaning process for the removal of residues. However, unlike product residues, it is expected that no (or for ultra sensitive analytical test methods - very low) detergent levels remain after cleaning. Detergents are not part of the manufacturing process and are only added to facilitate cleaning during the cleaning process. Thus, they should be easily removable. Otherwise, a different detergent should be selected.
c. Test Until Clean
Examine and evaluate the level of testing and the retest results since testing until clean is a concept utilized by some manufacturers. They test, resample, and retest equipment or systems until an "acceptable" residue level is attained. For the system or equipment with a validated cleaning process, this practice of re-sampling should not be utilized and is acceptable only in rare cases. Constant retesting and re-sampling can show that the cleaning process is not validated since these retests actually document the presence of unacceptable residue and contaminants from an ineffective cleaning process.
VII. BIBLIOGRAPHY
1) J. Rodehamel, "Cleaning and Maintenance," Pgs 82-87, University of Wisconsin's Control Procedures in Drug Production Seminar, July 17-22, 1966, William Blockstein, Editor, Published by the University of Wisconsin, L.O.C.#66-64234.
2) J.A. Constance, "Why Some Dust
Control Exhaust Systems Don't Work," Pharm. Eng., January-February, 24-26
(1983).
3) S.W. Harder, "The Validation of
Cleaning Procedures," Pharm. Technol. 8 (5), 29-34 (1984)
4) W.J. Mead, "Maintenance: Its
Interrelationship with Drug Quality," Pharm. Eng. 7(3), 29-33 (1987).
5) J.A. Smith, "A Modified Swabbing
Technique for Validation of Detergent Residues in Clean-in-Place Systems,"
Pharm. Technol. 16(1), 60-66 (1992).
6) Fourman, G.L. and Mullen, M.V.,
"Determining Cleaning Validation Acceptance Limits for Pharmaceutical
Manufacturing Operations," Pharm. Technol. 17(4), 54-60 (1993).
7) McCormick, P.Y. and Cullen, L.F., in
Pharmaceutical Process Validation, 2nd Ed., edited by I.R. Berry and R.A. Nash,
319-349 (1993)
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