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Cleaning Process Development and Validation

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Title: Cleaning Process Development and Validation

1
Cleaning Process Development and Validation

June 16, 2006
Brian Kim
VP of Quality
Tanox, Inc.

2
Part I
3
Regulatory/Compliance Overview

Applicable regulations and requirements
21 CFR 211.65 a)
Equipment . surfaces which contact components,
in-process materials, or drug products shall not
be reactive, additive or absorptive..
21 CFR 211.67
Equipment and utensil . cleaned, maintained, and
sanitized at appropriate intervals to prevent or
contamination that would alter the safety,
identity, strength, quality, or purity

4
Regulatory/Compliance Overview

21 CFR 211.182
Written cleaning Procedure
Cleaning and use log
Cholestyramine Resin USP recall due to the low
level contamination with intermediates and
degradants after reuse of recovered solvents from
pesticide production increased FDA awareness.

5
Regulatory/Compliance Overview

Guidance
Guide to Inspection for Validation of Cleaning
Processes. FDA, 1993
ICH Q7A, GMP for Pharmaceutical Active Ingredients

6
Regulatory/Compliance Overview

FDA 21 Century Risk-Based Quality System
Initiative
Define critical product attributes and control of
critical processes (Process Capacity) to ensure
SAFETY, PURITY, EFFICACY, QUALITY
Design Quality into processes
Science-based risk management
Real time QA

7
Cleaning Validation Overview

Objectives
Assurance of product purity, safety, efficacy and
quality
Prevention of product cross contamination by
byproduct, residual product, microbial residue
and residual detergent
When cleaning validation is required
Introduction of new equipment/product
Manufacturing/cleaning process changes
Raw material/cleaning agent changes

8
Cleaning Validation Overview

Good system design
Comprehensive Master Validation Program
Effective cleaning process development
Adequate analytical technique
Justifiable acceptance criteria product
specific (How Clean is Clean?)
Continuous data monitoring and evaluation
Acceptance criteria adjustment as necessary

9
Cleaning Validation Overview

Routine review of deviations, excursions and
change control related to cleaning process
parameters, equipment, and materials
Re-validation as required
Define what and how to revalidate
Define when to revalidate
Application of validation lifecycle management

10
Cleaning Validation Overview

Cleaning Validation Lifecycle Management

New product/Equipment
Evaluation of Cleaning Parameters
Cleaning Cycle Development
Validation Master Plan
Regular Data Review
(Re)Validation (IQ/OQ/PQ)
Routine Testing
11
Cleaning Cycle Development

Elements to consider
Design/Construction complexity of equipment
Characteristics of residuals/product to clean
Cleaning agents
Type of cleaning process (Automated vs. Manual)
Manufacturing process
Analytical methods and their sensitivity

12
Equipment Design/Construction for Effective
Cleaning

Adequate design/structural complexity and
configuration
Material and Surface
Non-Reactive and cleanability
Compatibility with detergents
Stage of Manufacturing Process
Upstream
Down stream Increased Risk
Drug product

13
Equipment Design/Construction for Effective
Cleaning

Structural/design complexity
Size and process piping configuration for CIP
Potential dead leg/space
Adequate turbulence
Adequate slope
Nozzle design and locations
Branch piping orientation

14
Equipment Design/Construction for Effective
Cleaning
Instrument Tee for CIP L/D lt1.5
D
L
Adequate turbulence (Flow rate) for CIP
5 ft/sec
½ ft/sec
5 ft/sec
15
Equipment Design/Construction for Effective
Cleaning
CIP Return
CIP Return
Bad
Good
16
Equipment Design/Construction for Effective
Cleaning
Branch piping orientation
Up
Parallel
Down
Good Design
Bad Design
17
Characteristics of Products

Understand (Bio)chemical characteristics of
Product(s)
Product matrix
Type of active molecule (e.g., protein, DNA,
peptide, small molecule)
Excipients/Process related components
Product matrix is a critical element for
Cleaning process design
For the determination of a detergent and process
parameters

18
Characteristics of Products

Physicochemical characteristics
Solubility with medium (e.g., water, organic
solvent)
Reactivity is a critical element for the
determination of process parameters
Degree of a reaction with a detergent or medium
at different conditions.
Degradants
Chemical state
Liquid
Semi-solid
Solid

19
Characteristics of Products

Microbe static property
Critical for detergent selection
Toxicity/Pharmacological potency
Critical for acceptance criteria
Potential product and/or component degradants
after reaction with a detergent
Critical for acceptance criteria

20
Cleaning Agent Selection

Selection of a Cleaning Agent
Depending on the particular type of chemicals
(soils) to remove considering
Chemical/Physical nature of the molecule (soil)
to remove
Reactivity
Physicochemical characteristics of the molecule
Chemical state of soils

21
Cleaning Agent Selection

Type of Detergent

22
Cleaning Agent Selection

Biological soils alkaline
Blending of other cleaning components with
alkaline detergent enhances cleaning effects.
Builders the group of complexing agents that
enhance the cleaning effect and the effect of
surfactant
EDTA, polyphosphate, NTA, citrates

23
Cleaning Agent Selection

Surfactants several types based on the ion
characteristics of the active group
Anionic, cationic, non-ionic and amphoteric
Anionic and Non-ionic used as components for
detergent
Cationic and amphoteric used in the formulations
of disinfectants for their microcidal effect
Surface tension capillary action

24
Cleaning Agent Selection

Complexing agents complexing with minerals and
inorganic components
Sequestering agent prevention of scale
formation (crystallization of water hardness)
May reduce the need for acid cleaning following
the base cleaning
Deformers
Oxidizing agents H2O2
Corrosion inhibitors - Silicates

25
Cleaning Agent Selection
Removed Soil
80 70 60 50 40 30 20 10 0
Cleaning agent Builder Surfactant
Single cleaning agent
Surfactant
Builder
0 2 4 6
8 10 12
14
Cleaning Time (mins)
26
Cleaning Agent Selection

Application parameters for cleaning agents
Type of cleaning agent
Depending on the type of soils to remove
Concentration
Effectiveness
EHS consideration
Temperature
Contact time

27
Cleaning Process Development

Selection of Cleaning Process
Automated vs. Manual
Automated CIP and/or COP
Consistency and reproducibility
Readily validatable
Better process control
Manual
Inconsistency
Hard to validate
Inadequate for most of the state-of-the-art
facilities

28
Cleaning Process Development

Consider
Historical cleaning data (trending)
Previous validation data if available
Complexity and delicacy of manufacturing
equipment
Level of facility automation
Cleaning cycle development
CIP or COP design and capacity
Nature of soils

29
Cleaning Process Development

Complexity and delicacy of equipment
Nature of product contacting surface
Sequence
Critical parameters
Legging time between the end of equipment use and
cleaning
Temperature
Pressure
Volume
Process time

30
Cleaning Process Development

Types of CIP (Clean-in-place)
Portable CIP
Simple control and non re-circulation
Multiple-Tank Re-use CIP
Separate tanks for detergents (Acid, Base) and
washing solution (e.g., water)
Re-circulation and re-use of detergents and
washing solution
May not be adequate for biopharmaceutical in
terms of prevent cross contamination (e.g., viral
contamination)

31
Cleaning Process Development

Single and multiple-tank single use CIP
Appropriate for Biopharmaceuticals
re-circulation
Relatively easy for validation but depending on
number of pumps, valves, and the complexity of
cycle
High degree of cycle flexibility
No re-use of cleaning agent for
biopharmaceuticals
Validation is depending on the complexity of the
cleaning sequence.

32
Cleaning Process Development

COP (Clean-out of place)
Used for miscellaneous fittings and parts out of
the main equipment (disassembly)
A single open tank for rinsing and washing
Re-circulation of detergent using a detergent
feed pump
Appropriate cycle development

33
Cleaning Process Development

Automated CIP system components and functions
Temperature sensors
Two for re-circulation system cleaning
solution supply and return monitoring
Temperature is a primary indicator of cleaning
cycle performance
Conductivity sensors
Detergent conc. monitoring
Conductivity a primary indicator of cleaning
cycle performance

34
Cleaning Process Development

pH sensors
Monitoring of rinsing efficacy
CIP supply flow sensors
Flow rate and totalization are directly related
to contact time
Magnetic flow sensors not recommended because
of inability to sense non-conductive fluid
CIP supply pressure sensors
Indicator of spray device performance and
solution contact time

35
Cleaning Process Development

CIP vessel level sensors
Indirect indicator of performance of the system
Return flow switch
Conductance based probe
Prevention of inadvertent events such as
mis-connection of supply and return circuits
product contamination
Spray device
Fixed and rotating

36
Safety
Part II
Purity
Efficacy
37
Cleaning Process Development

Sequence development
Pre-rinse piping and equipment to be cleaned by
pressure washing
End point
Total volume or time
On-line turbidity, conductivity or return flow
Must be drained or to kill-tank

38
Cleaning Process Development

Detergent washing
Acid or alkali depending on the type of soil
Continuous feed
Endpoint
Volume or time
Must be drained
Soaking with detergent as necessary
Chromatography system

39
Cleaning Process Development

Post rinse and drains
To remove residue after pre-rinse and detergent
washing
Continuous flow and drain
Usually not heated
Neutralization wash and drain
Endpoint total volume and/or elapse time
Final rinse and drain
Endpoint total volume and/or elapse time, pH,
conductivity

40
Cleaning Process Development

Parameter and range determination
Factoring experimental design (example)

41
Cleaning Process Development

Study approach
Coupon study
Same materials as manufacturing equipment
Equivalent surface treatment
Experimental run
Worst case approach
Residues to be cleaned
Equipment surface
Appropriate sampling and analytical methods

42
Cleaning Process Development

Sampling
Direct surface sampling
Selection of
Appropriate sample dissolving medium
Sample container
Sampling material(s)
Swab Interference by adhesive, Variability

Swabbing unidirectionally with a
new wet swab for each direction

Wet swab and finish with a dry swab

43
Cleaning Process Development

Rinse water sample
Dilution effect
Unreliable, inconsistent recovery
Visual inspection

44
Cleaning Process Development

Analytical Methods
Depending on the types of analytes
Proteins
Organic compounds
Inorganic compounds
Other biological contaminants
Adversary agents
Mycoplasma, virus
Residual host bacteria

45
Cleaning Process Development

Type of analytical methods
Specific
Multi-product equipment
Potent product
Toxic or potent degradants or contaminants
Non-specific
Broad application
Holistic evaluation
Selection of methods based on the nature of
analytes

46
Cleaning Process Development

Development of specific method(s) requires longer
time
Matrix of the material for method development
should be the representative of the cleaning
sample.
Inhibitory or enhance effects of the sample
matrix must be evaluated and appropriate sample
preparation and method should be developed.
Sensitive and specific

47
Cleaning Process Development

Selection of appropriate method(s) is a key for
successful cleaning validation
Routine and validation
Methods must be validated for
Sensitivity (LOD/LOQ)
Specificity
Precision
Accuracy

48
Cleaning Process Development

Examples of methods widely used in
biopharmaceutical cleaning process

49
Cleaning Process Development

Use methods in combination
Validation and routine cleaning sample analysis
Test intended routine cleaning samples during the
validation study and establish co-relationship
between specific and non-specific sample test
results. Use the ratio as a correction factor
during the routine cleaning sample analysis if
the results show relative difference in a
consistent manner.

50
Cleaning Validation

Validation Approach
Development of Validation Master Plan to
describe
Objective, scope, references, responsibilities
Nature of products (dosage form and therapeutic
areas) all products
Manufacturing process
Include equipment list
Cleaning system and process for each type of
equipment

51
Cleaning Validation

Validation Strategy
Multi-use vs. dedicated equipment
Individual vs. group vs. matrix
Scope of use vs. configuration
Each product basis vs. worst case approach
Define the worst case or group
Provide a scientifically sound justification if
chosen (e,g., degree of difficulty in cleaning,
toxicity)
List of Equipment and qualification status
Equipment PIDs
Cleaning system (e.g., CIP) qualification (I/OQ)
status

52
Cleaning Validation

Analytical method selection and validation
requirements
Recovery study requirements recovery factor
Determination of sampling methods
Lot requirements for validation
Documentation requirements
Protocol
Reports
Raw data
Re-validation requirements and frequency
Validation project planning (Generic)

53
Cleaning Validation

Cleaning Validation Prerequisites
Ensure that all cleaning process equipment are
adequately qualified.
Draft a cleaning SOP based on the development
study.
Prepare PID for each piece of equipment and
define sampling locations and/or methods.
Ensure that analytical methods are validated.

54
Cleaning Validation

Conduct a recovery study per type of equipment
construction material.
Protocol driven
Report recovery factor for each type of
equipment construction material
Define acceptance criteria.
Justification must be established.
Develop a detailed plan and responsibilities.

55
Cleaning Validation

Recovery study
Recovery rate is directly related to the
condition of equipment surface and sampling
technique.
Define appropriate sampling methods and
techniques.
Recovery factor must be reflected on the residue
calculation during the cleaning validation.

56
Cleaning Validation

Considerations for recovery study
Coupons and other materials
Representative of all types of equipment (316L
SS, Glass, plastic)
Same surface treatment (e.g., electropolishing)
Sampling materials
Sample container
Sampling methods
Spiking solution preparation
Simulated cleaning sample
Concentration should be at a level of acceptance
acceptance criteria

57
Cleaning Validation

Spiking and spiked coupon handling procedures
Clean coupons before spiking
Simulate actual cleaning condition
Allow the spiked solution to be on the coupon the
maximum time as cleaning time limit is defined
the SOP.
Evenly spike the solution on the defined area of
the coupon.
The coupon spiking area should be an equal to the
actual sampling area on the actual equipment.

58
Cleaning Validation

Coupon arrangement
Coupon to be arranged to have areas or separate
coupons for
Background blank
Control spiking sample prep solution
Sample spiking area
Sampling
Protocol and report
Define expected acceptance criteria
Example 60 120 RECOVERY
The recovery factor
Spiked value/recovered value

59
Cleaning Validation

Acceptance Criteria Approach
Visually cleanliness
Prerequisite of cleaning acceptance.
Cannot be an acceptance criterion alone.
Cleaning capability
Statistical analysis of historical cleaning data
Product specific data
Non-specific data (e.g, rinse water TOC) to be
evaluated based on the worst case (toxicity)
residual.
Data should be analyzed from the toxicity and
dosage level perspective

60
Cleaning Validation

Maximum daily dose based carryover
lt0.001 of any contaminant in maximum daily dose
of the subsequent batch (3 factors)
10 of maximum daily dose inactive
10 of maximum daily dose safety factor
10 of maximum daily dose cleaning capability
Toxicity based carryover
Toxicity data based criterion safety factor (1
10 of the toxicity) is applied to the toxicity.
Applicable to detergent, sanitizing agent and
cross-contaminating product.

61
Cleaning Validation

The lowest value to be chosen as acceptance
criteria.
Process capability to remove contaminants must be
considered.
Apply different criteria to different
manufacturing process step considering down
stream impurity/contaminant removal capacity.
The most stringent criteria to finished product
manufacturing.
Justification must be clearly documented.

62

Cleaning Validation

Acceptance criteria should include
Number of batches (consecutive)
Sample test time limit
Cleaning time limit (number of hours after
production)
Deviation handling
Allowed contaminant level per swab area or per
volume of sample

63
Cleaning Validation

Analytical Method Application
Non-specific method for the equipment at the
manufacturing step where the process material
matrix is complicated
Upstream Process (except viral particles)
Cell culture/fermentation media
By products
Cell debris
Nucleic acid
Assumption- the value represent the worst (the
most toxic) substance

64
Cleaning Validation

Contaminant specific (product specific) method
should be applied to multi-product down stream
equipment and finished product manufacturing
equipment
Rinse solution (water) test shall be performed
along with specific test
Rinse water test results are correlated to the
product specific test results and use the value
as a routine cleaning specification.

65
Cleaning Validation