Good manufacturing practices (GMP) require that a maximum acceptable holding period should be established to ensure that intermediates and bulk product can be held, pending the next processing step, without any significant adverse effect to the quality of the material. Such a holding period should be underwritten by data, but need not be extended to find the edge of failure for holding. WHO has published a guideline on Hold Time Studies.
A summary of the recommendations if given in the enclosed presentation prepared by “Drug Regulations”
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Hold Time Studies
1. This presentation is compiled by “ Drug Regulations” a
non profit organization which provides free online
resource to the Pharmaceutical Professional.
Visit http://www.drugregulations.org for latest
information from the world of Pharmaceuticals.
6/25/2015 1
2. This presentation is compiled from freely available
resources like the website of WHO , specifically
GENERAL GUIDANCE
ON “HOLD-TIME” STUDIES”
“Drug Regulations” is a non profit organization
which provides free online resource to the
Pharmaceutical Professional.
Visit http://www.drugregulations.org for latest
information from the world of Pharmaceuticals.
6/25/2015 2
Drug Regulations : Online
Resource for Latest Information
3. The World Health Organization (WHO) had released
the second draft of the guideline for the design of
hold-time studies in March 2015
The final version was released as a part of Technical
Report Series 992 (TRS 992, Annex 4) in June 2015.
This presentation is based on this final Guidance.
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4. Hold time
◦ Can be considered as the established time period for
which materials (dispensed raw materials, intermediates,
bulk, and finished products under quarantine) may be
held under specified conditions and will remain within
the defined specifications.
◦ The quality and stability of intermediate products, bulk
and finished products in quarantine should be ensured
at all stages of manufacture.
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5. Good Manufacturing Practices
◦ Manufacturers should ensure that the products they
manufacture are
Safe
Effective
Of the quality required for their intended use
Are consistently manufactured to
The quality standards appropriate to their intended use and
As required by the marketing authorization
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6. Good Manufacturing Practices
◦ Systems should ensure that Pharmaceutical products are
produced
According to validated processes
To defined procedures.
◦ Manufacturing processes should be
Capable
Consistent
Manufacture products of required quality
Manufacture products complying with their specifications
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7. Good Manufacturing Practices
◦ Arrangements should exist to ensure that the
Dispensed raw materials
Packaging materials
Intermediate products
Bulk and finished products
◦ are stored under appropriate conditions.
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8. Good Manufacturing Practices
◦ Storage should not have any significant negative effect on the
Processing
Stability
Safety,
Efficacy
Quality
of
◦ Materials
◦ Intermediate products
◦ Bulk products prior to final packing
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9. Good Manufacturing Practices Require that
◦ A maximum acceptable holding period should be
established
◦ Objective of Hold Time
To ensure that intermediates and bulk product can be held,
without any significant adverse effect to the quality of the
material till next step of processing
Such a holding period should be based on data
Studies need not be extended to find the edge of failure for
holding
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10. WHO guideline
◦ Focuses on hold-time studies for solid dosage forms
◦ Many of the principles can be applied to other dosage forms such as
liquids, creams and ointments
◦ Does not cover hold times in cleaning validation
◦ Does not cover manufacturing of active pharmaceutical ingredients (APIs)
or Biologicals
◦ Intended as a basic guide for use by pharmaceutical manufacturers and
GMP inspectors
◦ Does not intend to prescribe a process for establishing hold times,
◦ Reflects aspects that should be considered in the design of the hold-time
study
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11. Gather scientific and justifiable data to
demonstrate that the
◦ Dispensed raw materials and packaging materials,
intermediate and bulk products:
Remain of appropriate quality before processing to the
next stage;
Meet the acceptance criteria and release specification
for the finished product
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12. Collect data to justify the hold time during
◦ Development on pilot scale
◦ Process validation
◦ As part of an investigation of a deviation that
occurred during manufacture.
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13. Use a flow chart
Review manufacturing procedure
Break up the critical stages
Use time duration of each processing stage
Evaluate the potential impact of storage with
reference to environmental and storage
conditions.
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14. Processing Step Product
Binder preparation to granulation Granulate
Wet granulation to drying Dried Granules
Dried granules to lubrication/blending Lubricated Blend
Compression to coating Tablet cores
Coating solution to preparation Coating Solution
coating to packing Bulk coated Tablets
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For oral tablets the following stages may be considered:
15. Prepare a written protocol
Include following in protocol
◦ Activities to be performed
◦ Test parameters
◦ Acceptance criteria appropriate to the material or
product under test
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16. ◦ Title
◦ Reference number
◦ Version
◦ Date
◦ Objective
◦ Scope
◦ Responsibility
◦ Procedure
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◦ Description of the
material/product;
◦ Sample quantities;
◦ Sampling method and
criteria;
◦ Acceptance limits;
◦ Frequency for sampling;
◦ Sampling locations;
◦ Pooling of samples;
The protocol and report should generally include the following
◦ Storage conditions
◦ Type of container
◦ Methods of analysis
◦ Results
◦ Conclusion
◦ Recommendation
◦ Signatures and dates
17. Acceptance criteria are typically more stringent than registered
specifications,
This provides assurance that the material is well within control.
Consider any known stability trend when setting the specifications
Consider microbiological aspects for certain type of products
Use validated stability indicating methods for testing of bulk
intermediates and product
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18. Use one or more batches of a material, intermediate or product for
determining hold times.
Use a risk-based approach to determine the appropriate number of
batches
Consider the characteristics of the materials and other relevant
aspects.
Hold for defined period a representative sample of the batch of
material or product subjected to the hold-time study
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19. Use one or more batches of a material, intermediate or product
Use a risk-based approach to determine the number of batches
Hold a representative sample for the defined hold period.
Keep the material in either original or simulated container
Containers used should be the same pack as used in production
If the pack is exceptionally large use a equivalent
◦ same material of construction and closure system to the production
packaging system
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20. Reducing the size of container when necessary for
testing holding time, should be justified.
Where head space is important use maximum head
space (worst-case scenario) situation
In such cases, the ratio of headspace to contents in
the test containers should be at least as great as the
maximum that is possible in routine production
(especially taking into account part-filled containers).
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21. Store samples in same environmental
conditions as in manufacturing / storage
Establish a sampling plan
Calculate required sample amount based on
the batch size, the intervals and tests to be
performed.
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22. Keep the sample in storage container and test it
Compare results with the initial baseline data of the
control sample
Samples may be pooled for analysis where
appropriate
Where necessary, individual samples may be tested
and compared
Identify trends & justify limits with Statistical analysis
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23. Batches of products subjected to a hold-time study should be
considered for long-term stability testing if data show trending or
shifting patterns during the intermediate time periods up to the end-
time.
The shelf-life of the product – irrespective of hold times should be
measured from the time the actives are mixed with other ingredients.
Normally intermediate and bulk products should not be stored beyond
the established hold time.
All testing of bulk intermediates and product should be performed using
validated stability indicating methods.
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24. 6/25/2015 24Drug Regulations : Online Resource for Latest Information
Stage Test Time Period for
Testing
Binder Preparation
including
granulation pastes,
coating solution
and coating
suspension
Physical
appearance
Specific gravity
Viscosity
Sedimentation
pH
Microbial test
Initial, 12, 24,
36, 48, 60, 72
hours
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Stage Test Time Period for
Testing
Granules Description
Assay
Moisture content
(loss on drying)
Water content
Particle size
distribution
Bulk density
Tap density
Angle of repose
Initial, 15th
day, 30th day,
45th day
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Stage Test Time period for
Testing
Blend Microbial test
Moisture content
(loss on drying)
Blend uniformity
Particle size
Bulk/tapped
density
Initial, 15th day,
30th day, 45th
day
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Stage Test Time period for
Testing
Core tablets –
uncoated (in
bulk
containers)
Description
Hardness
Thickness
Friability
Appearance
Dissolution
Disintegration
Assay
Degradation
products/related
substances
(where applicable)
Uniformity of dosage
units
Microbial test
Initial, 30th day,
45th day, 60th
day and 90th day
28. Examples of stages and tests that may be considered.
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Stage Test Time Period for
Testing
Coated tablets (in bulk
containers)
Description
Hardness
Thickness
Friability
Appearance
Dissolution/dissoluti
on profile
Disintegration
Assay
Degradation
products/related
substances
(where applicable)
Uniformity of dosage
units
Moisture content
Microbial test
Initial, 30th day,
45th day, 60th day
and 90th day
29. This presentation was compiled from freely
available resources like the website of WHO ,
specifically GENERAL GUIDANCE
ON “HOLD-TIME” STUDIES”
“Drug Regulations” is a non profit organization
which provides free online resource to the
Pharmaceutical Professional.
Visit http://www.drugregulations.org for latest
information from the world of Pharmaceuticals.
6/25/2015 29
Drug Regulations : Online
Resource for Latest Information