1. QC/QA Mary Malarkey
Director, Division of Case Management
Office of Compliance and Biologics Quality
Center for Biologics Evaluation and Research
March 21, 2001
2. QC/QA = CGMP Preparation of products for administration to humans, including clinical trials
GLPs are not GMPs
CGMPs cover manufacturing, controls, testing and documentation
Difference between Quality Assurance and Quality Control not addressed
3. Quality Control Unit� 21 CFR 211.22 Approve/reject all components, intermediates, products
Approve/reject procedures/specifications
Review records; ensure investigations are conducted
Adequate laboratory facilities for testing
Responsibilities and procedures in writing
(Should be independent from production)
4. QC vs. QA� proposed revision to 211 Some confusion over QC vs. QA (names, functions, requirements)
QC - generally testing activities to assure that specifications adhered to
QA- oversight responsibilities (“the QC of QC”) - auditing methods, results, systems and processes; trending
5. Other Regulations Good Laboratory Practices
21 CFR 58.35 “Quality Assurance Unit…..shall be responsible for monitoring each study to assure management that the facilities, equipment, personnel, methods, practices, records and controls are in conformance with the regulations in this part….shall be entirely separate from and independent of the personnel engaged in the direction and conduct of the study.”
6. Other Regulations Good Tissue Practices (proposed rule)
21 CFR 1271.3(oo) - “Quality Program…This program includes preventing, detecting and correcting deficiencies that may lead to circumstances that increase the risk of introduction, transmission, or spread of communicable disease.”
7. QC and QA�Dear Sponsor Letter 3/6/2000 Summary of QC/QA programs. Brief description of system for preventing, detecting and correcting deficiencies that may:
compromise product integrity or function
lead to possible transmission of adventitious infectious agents
8. QC and QA: �Dear Sponsor Letter Identify each individual who has authority over the QC/QA program(s)
Provide date of last QC/QA audit of:
your operations
contract manufacturers, vendors and other partners
9. QC and QA: � Dear Sponsor Letter Unique considerations for these products:
QC and/or QA may be one individual
most “QC”, that is testing, may be contracted out;
most validation/qualification activities contracted out;
many vendors involved, e.g. water, media
facility may be used by multiple sponsors
10. General Considerations DOCUMENTATION - approval/review
Batch Production Records (211.188 & 211.192)
Equipment - cleaning and use (211.182)
Laboratory Records (211.194)
Standard Operating Procedures (211.100)
“Distribution” Records (211.196)
Complaint Files (211.198)
SHOULD ALLOW TRACEABILITY
11. Prevent Deficiencies - 1 Testing of all cell and viral banks
review of SOPs, protocols, results from test lab
Testing, or certification, of components
example; media -> animal derived materials BSE free countries (1/6/98 FR notice)
Screening of patients or use of universal precautions
12. Prevent Deficiencies - 2 Facility
adequately designed, validated
equipment calibrated, qualified, certified
maintenance and monitoring procedures
requalification procedures in place
cleaning procedures in place for equipment and facility (variety of cleaning agents)
segregation procedure in place
13. Prevent Deficiencies - 3 Manufacturing process (vector and product)
controls developing
validation of aseptic processes
operator training and qualification
procedures for deviations from process or other deviations associated with production
testing of product; review of all records associated with lot - > release
14. Detection Considerations Monitoring
facility
personnel
Testing
components
in-process
final product
Trending
15. Correction Considerations
Importance of traceability
Procedures for investigations (211.192) should extend to other lots of product
Procedures for corrective actions
Procedures for handling of complaints or AEs that may be associated with manufacturing
Procedures for notification
16. Examples -1 Sterility test failure
perform identification
review records on components
review records on equipment cleaning and use
review environmental and personnel monitoring records
17. Examples - 1 Isolate identified as S. epidermidis
Personnel monitoring result - same organism
Retrain and requalify operator
Increase routine monitoring of operator
18. Examples - 2 (actual) Mold contamination of in-process cells
investigation inconclusive
Mold contamination of in-process cells
trace both flasks to shelf in incubator
monitor incubator
isolate same mold
Corrective action - addition of fungicidal agent (was using only IPA)
19. Description of Program Should hit on points previously described which should ensure prevention, detection and correction of deficiencies that may compromise product.
Distinguish between testing (QC) and oversight (QA) activities
20. Identification of Authority Should be separate from “production” which is sometimes the sponsor
Should have ultimate authority to release/reject, i.e. shouldn’t be producing, testing, reviewing, releasing
Ideal - separate unit with ultimate reporting to sponsor, but authority, i.e, sponsor should accept decision
21. QC/QA Audits Date of last audits for the following should be provided…….
Later paragraph suggests that a plan for audits should be in place: what needs to be audited, how audited, frequency of audits
22. QC/QA Audits Manufacturing operations (211.180)
annual
representative number of batches
all associated records and deviations, complaints
responsible individual must be notified of results
23. QC/QA Audits Vendors (211.84)
could be quite an undertaking given number of components; audit may entail testing of certain lots of components to ensure C of A accurate. Certification by vendors.
Contract Manufacturers
most likely testing - cell and viral banks, final product; should be reviewing and approving SOPs, validation protocols used
24. QC/QA Audits Contract Validation Activities
should be involved in plans and implementation
should “pick up ball,” that is, maintain validated state through proper monitoring and maintenance activities
revalidation/requalification/recertification programs
25. Conclusion Sponsors should be in compliance with CGMPs with respect to QC/QA functions
Problem areas:
Lack of documentation
Lack of traceability
No separation between QC/QA and other operations
26. Mary Malarkey
OCBQ/DCM
301-827-6201
