Title: GOOD MANUFACTURING PRACTICES IN A QUALITY WORLD
1GOOD MANUFACTURING PRACTICESIN A QUALITY WORLD
- Gordon Harnack
- President, Oracle Consulting Group
- Tucson, AZ
www.fdamaze.com
2The Discussion Plan
- Definitions
- General Discussion
- Drugs
- Devices
- In Vitro Diagnostics
- Food
- Cosmetics
- GMP Specifics Device GMPs
3What are Good Manufacturing Practices (GMP)?
- Good Manufacturing Practice regulation is a set
of regulations, codes, and guidelines for the
manufacture of drugs (known as medicinal products
in Europe), medical devices, diagnostic products,
foods products and Active Pharmaceutical
Ingredients (APIs). - http//en.wikipedia.org/wiki/Good_Manufacturing_Pr
actice
4What are Current Good Manufacturing Practices
(cGMP)?
- Good Manufacturing Practice implemented in 1976
for the manufacture of products that are under
FDA jurisdiction, including pharmaceuticals,
biological products and medical devices. Current
Good Manufacturing Practice ensures that finished
products have the correct identity, strength,
quality and purity characteristics they are
represented to have, and have not been altered
during processing, packaging, or handling. It
requires extensive use of documentation and
strict reconciliation of inventory. - www.sciteclabs.com/dictionary.html
5Why GMP Regulations?
- The Federal Food, Drug Cosmetic Act authorizes
such regulations - Title 21, Chapter 9, FFDC Act has 17 references
to GMPs - FDAs mechanism to implement oversight of any
manufacturing operation - Establishes FDAs minimal manufacturing control
expectations - Make management the chief jailable officer
- Absent GMP regulations fall back on FFDC Act!
6FDAS ExpectationsRelated to Firm Size
- The larger the firm the greater FDA expectations
- However, even the smallest firm MUST address
every aspect of applicable FDA regulations.
7What FDA Centers deal with Drug GMPs?
- Center for Biologics Evaluation Research (CBER)
- Center for Drug Evaluation Research (CDER)
- Center for Veterinary Medicine (CVM)
- CDER states Useful to manufacturers of
components used in the manufacture of these
products
8What Types of Firms are Exempt from Drug GMPs?
- Drug wholesalers, retailers, pharmacies
hospitals unless engaged in manufacturing
operations beyond the usual dispensing or selling
of drugs at retail - Compounders of drugs pharmacists physicians
- Note Compounded drugs must still be composed of
FDA approved components. - Note Some products are exempt from certain
elements of Drug GMP.
9What Types of Firms are Exempt from Drug GMP
Regulations? (cont)
- Manufacturers of active pharmaceutical
ingredients (APIs) bulk drugs are exempt from
cGMP REGULATIONS but NOT cGMP requirements of the
FFDC Act! - FDA cites API manufacturers for violations of the
ACT, not drug GMP regulations - FDAs GMP regulations are used as guidance
during inspections. - FDA claims to be working on specific API GMPs
10Drug GMPs Apply to
- Prescription OTC drugs, including homeopathic
drugs - Manufacturing facilities of ALL sizes
- Investigational drugs for clinical trials
- Foreign produced drugs distributed in the U.S.
11Drug GMPs
- 21 CFR 210 - cGMP in Manufacturing, Processing,
or Holding of Drugs General - 21 CFR 211 - cGMP Practice for Finished
Pharmaceuticals - 21 CFR 210 211 300 shalls
12Drug GMPs (continued)
- Applicability
- GMP of s 210 226 s 600 680 supplement
not supersede each other, unless otherwise
directed - Compliance failures ? adulterated drug product
13Drug GMPs (continued)
- Proposed new drug cGMPs will model FDAs intent
to integrate QS RISK MANAGEMENT to harmonize
with other non-drug regulatory systems ISO 9000 - FDA states that a robust modern QS must embrace
the concept that - Quality should be built into the product, and
testing alone cannot be relied on to ensure
product quality.
14Drug GMPs (continued)
- GMP Regulations specific to CBER regulated
products - 21 CFR 606 Current GMP for blood blood
products - 21 CFR 610 General biological products
standards - 21 CFR 630 General requirements for blood,
blood components blood derivatives - 21 CFR 640 Additional standards for human blood
and blood products - 21 CFR 660 Additional standards for diagnostic
substances for laboratory tests - 21 CFR 680 Additional standards for
miscellaneous products
15Medical Device GMPs
- QUALITY SYSTEM REGULATIONS
- 21 CFR 820 - 200 shalls
- Control each phase of manufacturing
- Harmonized with ISO 9000
- Greater emphasis on compliant handling,
corrective preventive actions, labeling
16What Types of Firms are Exempted from Device GMPs?
- Component manufacturers
- Note Some individual TYPES of devices are
exempt from some elements of GMP regulations, for
example - Many Class I devices, like tongue depressors,
are typically exempted from all GMPs except
records (820.180) complaint files (820.198).
17In Vitro Devices GMPs
- 21 CFR 809 In vitro diagnostic products for
human use - approximately 25 shalls
18Cosmetic GMPs No Specific GMP Regulations
- Regulated under the FFDC Act for
- Labeling
- Ingredients
- Contaminants
- Processing
- Packaging, or
- Shipping and handling
19Current Good Food Manufacturing Practices
- 21 CFR 110 approximately 95 shalls
- Focus on
- Sanitary/Unsanitary conditions
- Personnel, Equipment Buildings
- Production/Process Controls
- Raw materials
- Water
- Storage
- Warehousing distribution
20Now a Close Examination of Medical Device GMPs
21What Types of Firms are Subject to Device GMPs?
- Remanufacturers
- Custom Device Manufacturers
- Contract Manufacturers
- Contract Testing Labs
- Repackagers, Relabelers Specification
Developers - Manufacturers of Accessories
- Initial Distributors
22Medical Device GMP20 Elements
- Labels Labeling
- Acceptance controls
- Non-conforming product controls
- Corrective preventive action controls
- Handling, storage, packaging, preservation
delivery controls - Quality record controls
- Installation Servicing controls
- Complaint Handling controls
- Statistical technique controls
- Management responsibility
- Quality system controls
- Training controls
- Design/Development controls
- Document data controls
- Purchasing controls
- Product identification traceability controls
- Process and manufacturing controls
- Inspection testing controls
- Inspection, measuring, test equipment controls
- Process Validation
23Management Controls
- Management shall
- Establish its policy and objectives for, and
commitment to quality - Policy is understood
- Implemented
- Maintained at all levels
- Establish maintain adequate organizational
structure ensuring that devices are designed
produced in regulatory compliance - Establish maintain appropriate responsibility,
authority interrelations of all personnel - Provide adequate resources
- Appoint a Management Representative
24Management Controls (continued)
- Management shall
- Require the Management Representative to review
the suitability effectiveness of the QS at
defined intervals to ensure - Establish a quality plan that defines quality
practices, resources activities - Establish how requirements for quality are met.
- Establish maintain QS procedures
25Quality System Controls
- Establish procedures for quality audits
- Sufficient personnel with necessary education,
background, training experience to
26Training Controls
- Establish procedures to identify training needs
ensure all personnel are trained to adequately
perform their assigned responsibilities - Personnel shall be made aware of device defects
which may occur from improper performance - Personnel performing verification/validation
activities shall be made aware of defects
errors that may be encountered
27Design Controls
- Planning
- Requirements
- Specifications
- Verification
- Validation
- Change Control
- Review
- Transfer
- Design History File (DHF)
28Design Risk Analysis
- Safety requirements should be commensurate with
the hazards that can result from a system
failure. - FDA expects that all individual hazards,
including SW, be identified and either eliminated
or reduced to acceptable levels during the
devices design development - FMEAs Fault Trees
29Document Data Controls
- Establish Maintain procedures (EMP) to control
ALL documents required by regulationsincluding - Document review, approval distribution
- Document changes
30Purchasing Controls
- EMP to ensure that ALL purchased or otherwise
received product services conform to SPECIFIED
REQUIREMENTSincluding - Evaluation of suppliers, contractors
consultants - Establish maintain data that clearly describe
or reference SPECIFIED REQUIREMENTSincluding
quality requirements
31Product ID Traceability Controls
- EMP for identifying product during ALL stages of
receipt, production, distribution installation - Devices intended for surgical implant, life
sustaining or supportingwhose failure when
properly used can be expected to result in
significant injury shall be identified with a
control number
32Process Manufacturing Controls
- Manufacturer shall develop, conduct, control
monitor production processes to ensure that a
device conforms specifications - Establish maintain process control procedures
that describe all necessary controls
33Production Process Controls (continued)
- Process controls shall include
- Documented instructions, SOPs, methods that
define control production - Monitoring control of process parameters,
component device characteristics - Compliance with specified standards or codes
- Approval of processes equipment
- Criteria for workmanship expressed in documented
standards or by identified approved samples
34Production Process Controls (continued)
- EMP to control ALL changes to specifications,
methods, processes or procedures - Where environmental conditions can have any
adverse effect on product qualityEMP to
adequately control those conditions - EMP for health, cleanliness, personnel practices
clothing of personnel
35Production Process Controls (continued)
- EMP to prevent contamination of equipment or
product - Provide buildings of suitable design with
sufficient space to perform necessary operations,
prevent mix-ups assure orderly handling
36Production Process Controls (continued)
- Ensure that ALL equipment used in manufacturing
process meets its specified requirements - Equipment is properly installed, maintained,
adjusted, cleaned used - Establish maintain schedules for equipment
adjustment, cleaning or other maintenance - Conduct periodic inspections
- Ensure limitations/tolerances are posted
37Production Process Controls (continued)
- Where manufacturing material could be expected to
have adverse effectsEMP for the use removal of
those materials - Validate any computers or automated data
processing systems used
38Inspection Testing Controls
- Manufacturers shall ensure that ALL inspection,
measuring test equipment is suitable is
capable of producing valid results - EMP to ensure equipment is routinely calibrated,
inspected, checked maintained
39Inspection, Measuring Test Equipment Controls
- Calibration procedures shall include specific
directions limits for accuracy precision - Accuracy precision failures shall require
remedial action to reestablish the limits
assess adverse effect(s) on product quality - Calibration standards used shall be traceable
- Calibration records shall include equipment ID,
dates, individuals, the next calibration date
40Process Validation
- Where the results of processes cannot be FULLY
verified by inspection test, the process shall
be validated according to established procedures - EMP to monitor control validated process
parameters, controlling - Personnel, records changes
41Label, Labeling Packaging
- EMP to control labeling activities, including
label - Integrity
- Inspection
- Storage
- Operations
- Control number
42Packaging
- Manufacturer shall ensure that packaging
shipping containers are designed constructed to
protect the device from alteration or damage
43Acceptance Controls
- EMP for inspections, tests or other verifications
as acceptance of - Incoming product against specified requirements
- In-process product against specified requirements
- Finished devices to ensure EACH production run,
lot or batch meets acceptance criteria
44Acceptance Controls (continued)
- Manufacturer shall
- Document acceptance activities, including
- Activities performed
- Dates
- Results
- Signatures of individuals
- If appropriate, equipment used
- Identify acceptance status throughout the
processes..
45Non-conforming Product Controls
- EMP to control non-conforming product (NCP)
- Procedures shall control ID, documentation,
evaluation, segregation disposition of NCP - Evaluation shall include determining any need for
an investigation the persons/organizations
responsible for the NCP
46NCP Controls (continued)
- EMP that define the responsibility for review
the authority for the disposition of NCP - Procedures shall control
- Reviews dispositions
- Records shall document any justification for use
of NCP signatures of authorizers - Rework shall include appropriate retesting,
reevaluation adverse effects assessment to
ensure the product meets specifications
47Corrective Preventive Action Controls
- EMP for implementing CAPAs, including
- Analyzing processes, work ops, concessions,
audits, records, complaints, returns, other
sources of quality data - Use of appropriate statistical methods
- Investigating nonconformances to product
processes the QS - Identifying action(s) needed to correct or
prevent recurrence of nonconformances
48CAPA Controls (continued)
- CAPA procedures shall require
- Verification or validation of CAPAs to ensure
their effectiveness that they do not adversely
affect the finished device - Implementing recording changes in methods
procedures needed to correct prevent quality
problems - Ensuring information identified is disseminated
to all appropriate individuals - Submitting records for management review
49Handling, Storage, Preservation Delivery
Controls
- EMP to
- Control storage areas to prevent mix-ups, damage,
deterioration, contamination or other adverse
effects - Control product requiring stock rotation
- Control receipt from dispatch to storage areas
50Delivery Controls
- EMP to
- Ensure only approved devices are released
- POs are reviewed to ensure ambiguities errors
are resolved - Ensure stock that deteriorates over time is
properly controlled expired devices are not
distributed - Maintain distribution records that ID
- Name address of initial consignee
- Date, ID quantity of devices shipped
- Any control numbers used
51Quality Record Controls
- All required records shall be maintained at the
manufacturing location or other location that is
reasonably accessible for FDA inspection, review
copying - Records deemed confidential may be so marked
- All required records shall be retained for the
devices expected life but in no case less than
2 years from the date of release
52Quality Records Quality System Records (QSR)
- Manufacturers shall maintain a quality system
record (QSR) that includes - Procedures and records of activities required by
FDA regulation that are not specific to a
particular type of device, including - SOP creation numbering SOPs
- Training SOPs and records
- Purchasing SOPs and records
- Supplier assessment SOPs and records
53Quality Records Device Master Record (DMR)
- Maintain an approved DMR, including
- Device specifications drawings, composition,
formulation, component specifications SW
specifications - Product process specifications equipment specs,
production methods, production SOPs
environmental specs - QA SOPs, QA specs, acceptance criteria QA
equipment - Packaging labeling specs, methods
- Installation, maintenance servicing SOPs
54Quality Records Device History Record (DHR)
- EMP that ensure the DHR documents devices were
manufactured in accordance with the DMR FDA
regulations, the DHR includes - Date(s) quantity of manufactured devices
- Quantity released for distribution
- Acceptance records
- Primary ID label labeling
- Any device ID control number(s) used
55Installation Servicing Controls
- EMP for adequate installation, inspection
instructions any needed test activities - Procedures shall ensure proper installation
device performance after installation - Installation SOPs shall be distributed
appropriately
56Installation Servicing Controls
- Procedures shall require
- Installation personnel perform any required
testing in accordance with manufacturers
instructions document the inspection testing
to demonstrate proper installation - Specified servicing requirements follow
established maintained SOPs that require
servicing meets specified requirements - Service reports are analyzed with appropriate
statistical methods
57Servicing Controls
- Service reports that represent an event that must
be reported to FDA under MDR regulations shall
automatically be considered a complaint handled
in accordance with FDA complaint handling
regulations - Reports shall include
- Name, date, ID any control of devices
serviced - Individual performing service service performed
- Any test inspection data
58Complaint Handling Controls
- EMP for
- Receiving, reviewing evaluating complaints by a
FORMALLY DESIGNATED UNIT - Complaints shall be
- Processed in a uniform timely manner
- Oral (complaints) documented upon receipt
- Evaluated to determine if complaint represents an
MDR event requiring reporting
59Complaint Handling Controls (continued)
- Manufacturers shall
- Review evaluate all complaints to determine if
an investigation is necessary - If a determination is made that no investigation
is required, a record of shall be made that IDs
the reason the individual making the decision
60Complaint Handling Controls (continued)
- Complaints involving device failures to meet ANY
specification shall be - Reviewed, evaluated investigated unless such
investigation has already been performed for a
similar complaint another investigation is
unnecessary - Documented to show a determination of
- Whether the device failed to meet specifications
- Whether the device was being used for treatment
or diagnosis - Any relationship to any device to any reported
incident or adverse event
61Complaint Handling Controls (continued)
- Complaint investigation records shall include
- Device name date complaint received
- Device ID control s used
- Name, address phone of complainant
- Nature details of complaint
- Dates results of investigation
- Any corrective action taken
- Any reply to complainant
62Statistical Technique Controls
- Where appropriate, EMP for
- Identifying valid statistical techniques required
for establishing, controlling verifying the
acceptability of process capability and product
characteristics - Sampling plans, when used, shall be written
based on valid rationale - Ensuring sampling methods are adequate for their
intended use
63Useful Tools in Understanding GMPs
- Warning Letters Recall postings
- Guidance Documents
- Compliance Policy Guides (CPGs)
- Compliance Program Guidance Manual (CPGM)
- Guidance Documents for Regulated Industry
- Regulatory Procedures Manual (RPM)
- Investigations Operations Manual
- Laboratory Information Bulletins
- Laboratory Procedures Manual
64One Final Note
- FDA is NOT ALWAYS RIGHT!
- The Agency is made up of PEOPLE, people with
strong convictions egos - The Agency is a bureaucracy bureaucracies
over-reach, over-state, over-react almost NEVER
admit they are wrong - The following is an example of a bureaucratic
mis-step.
65One Final Note (continued)
- Between 2001 2004 Utah Medical was cited by FDA
for a number of GMP violations - August 2004 FDA sought a Permanent Injunction to
stop the firm from manufacturing distributing
medical devices UNTIL the firm DEMONSTRATED
corrections in deviations from GMPs - "FDA will not tolerate manufacturing practices
that can potentially put patients at risk," said
FDA Acting Commissioner Dr. Lester M. Crawford
66One Final Note (continued)
- FDAs injunction followed three years of FDA
inspections that FDA claimed revealed a pattern
of significant deviations from the Quality System
regulation at Utah Medical's Midvale facility. - FDA claimed Utah Medical has consistently failed
to ensure that its products are manufactured in
accordance with the Quality System regulation.
67One Final Note (continued)
- On Oct 21, 2005 Federal Judge Bruce Jenkins found
stated This is an unusual case. The safety of
the products manufactured by Utah Medical has
never been at issue.
68One Final Note (continued)
- The judge noted that Even though product safety
is a non-issue, the relief originally sought by
the United States was to stop Utah Medicals
products from entering commerce because of
alleged persistent deficiencies of Utah Medical
in complying with the applicable quality system
regulations (21 CFR 820), and asserting that a
failure to comply by definition produced an
adulterated product and subjected the product and
the persons responsible for the product to
regulatory action.
69One Final Note (continued)
- Judge Jenkins went on to state In short, the
United States asked that Utah Medical be ordered
to stop the sale of product until Utah Medical
complies with the regulation 21 CFR 820 and in
a manner that has been found acceptable to FDA. - Further he stated The court has been impressed
as well by Utah Medicals design of product, its
record-keeping of each step along the way, the
acceptance in the market of its products, the
Companys uniform processing of complaints, and
the manner in which change is made in practice
and procedure as a result of complaint handling.
70One Final Note (continued)
- Judge Jenkins concluded It makes no sense for
the court to order Utah Medical to do something
they are already doing. - The Court disagreed with all allegations by the
FDA, and dismissed the lawsuit filed in August
2004 that sought to shut down UTMD, without any
evidence of unsafe, ineffective, or defective
products or products causing any patient harm,
until UTMD complied with the FDAs interpretation
of the QSR, an interpretation that was never
provided to UTMD until after the lawsuit was filed
71One Final Note ( continued)
- The U.S. Federal District Court in Salt Lake City
confirmed that UTMD is operating in compliance
with 21 CFR 820, the U.S. Food Drug
Administration (FDA) Quality System Regulation
(QSR).
72Questions
73Abbreviations Used
- - Paragraph
- APIs - Active pharmaceutical ingredients
- CAPA Corrective Action Preventive Action
- CBER Center for Biologics Research
Development - CDER Center for Drug Evaluation Research
- CDRH Center for Devices Radiologic Health
- CVM Center for Veterinary Medicine
- CFR Code of Federal Regulations
- cGMP Current Good Manufacturing Practice
- CPGs Compliance Policy Guides
- CPGM Compliance Program Guidance Manual
- DHF Design History File
- DHR Device History Record
- DMR Device Master Record
- FDA Food Drug Administration
- FDA Food Drug Administration
- FFDC or FFDC Federal Food Drug Compliance
(Act) - FMEA Failure Mode Effects Analysis
- EMP Establish maintain procedures
- GMP Good Manufacturing Practice
- ID - Identification
- ISO Acronym for International Standards
Organization - OTC Over the Counter
- NCP Nonconforming Product
- QA Quality Assurance
- QS Quality System
- QSR Quality System Regulation
- SOP Standard Operating Procedure
- UTMD Utah Medical Device