Committee For Proprietary Medicinal Products (CPMP) : Inspections
Committee For Proprietary Medicinal Products (CPMP) : Inspections
Committee For Proprietary Medicinal Products (CPMP) : Inspections
Inspections
Note:
This guideline includes a minor correction to the earlier version CPMP/QWP/122/02 corr. and
CPMP/QWP/122/02, which came into operation in June 2003. CPMP/QWP/122/02 replaced
CPMP/QWP/556/96. See revision history for details.
The guideline CPMP/QWP/556/96 was given a new number CPMP/QWP/122/02 and revised
to be brought in line with the requirements of the Note for Guidance on Stability Data
Package for Registration in Climatic Zones III and IV (CPMP/ICH/421/02), the Note for
Guidance on Stability Testing of New Drug Substances and Products
(CPMP/ICH/2736/99 corr) and the Common Technical Document (CPMP/ICH/ 2287/99).
Within the EU, data from studies generated using the new conditions are accepted
immediately. Furthermore, data from studies where the relative humidity has been changed
from 60 % RH to 65 % RH during the study to meet the new requirements will also be
accepted under the condition that the respective storage conditions and the date of the change
are clearly documented and stated in the application file.
It is recommended that all marketing authorisation applications contain data from complete
studies at the intermediate storage condition 30 °C ± 2 °C/65 % RH ± 5% RH, if applicable,
by February 2006.
The following guideline is an extension of the Note for Guidance on Stability testing of New
Drug Substances and Products (CPMP/ICH/2736/99 corr) and sets out the stability testing
requirements for existing active substances and related finished products. For the purposes of
this guideline, an existing active substance is one that has been authorised previously through
a finished product within the European Community1.
This guideline is applicable to chemical active substances and related finished products,
herbal drugs, herbal drug preparations and related herbal medicinal products and not to
radiopharmaceuticals, biologicals and products derived by biotechnology.
The guideline seeks to exemplify the core stability data package required for such active
substances and finished products, but leaves sufficient flexibility to encompass the variety of
different practical situations that may be encountered due to specific scientific considerations
and characteristics of the materials being evaluated. Alternative approaches can be used when
there are scientifically justifiable reasons.
The purpose of stability testing is to provide evidence on how the quality of an active
substance or finished product varies with time under the influence of a variety of
environmental factors such as temperature, humidity, and light, and to establish a re-test
period for the active substance or a shelf life for the finished product and recommended
storage conditions.
The choice of test conditions defined in this guideline refers to the Note for Guidance on
Stability testing of New Drug Substances and Products (CPMP/ICH/2736/99 corr).
1
This approach is consistent with the definition of new active substance provided for under Part B of the
Annex to Council Regulation 2309/93 as follows: substance not authorised by any Member State on 1.1.95
for use in a finished product intended for human use.
2.1.1 General
Information on the stability of the active substance is an integral part of the systematic
approach to stability evaluation.
For active substances not described in an official pharmacopoeial monograph (European
Pharmacopoeia or the Pharmacopoeia of a European Union Member State) stability studies
are required.
For active substances described in an official pharmacopoeial monograph (European
Pharmacopoeia or the Pharmacopoeia of a European Union Member State), which covers the
degradation products and for which suitable limits have been set but a re-test period is not
defined, two options are acceptable:
a) The applicant should specify that the active substance complies with the
pharmacopoeial monograph immediately prior to manufacture of the finished product.
In this case no stability studies are required on condition that the suitability of the
pharmacopoeial monograph has been demonstrated for the particular named source
(refer to the Note for Guidance on Summary of Requirements for Active Substances in
Part II of the Dossier (CPMP/QWP/297/97));
b) The applicant should fix a re-test period based on the results of long term testing, taking
the results of testing under accelerated or, where applicable, intermediate storage
conditions, into consideration (see 2.1.7 Storage Conditions).
In the case of herbal medicinal products, active substances include herbal drugs and herbal
drug preparations. Herbal drugs which are used as starting material in the manufacturing
process for a herbal drug preparation shall comply with specification before use (e.g. before
extraction).
Stress testing of the active substance can help identify the likely degradation products, which
can in turn help establish the degradation pathways and the intrinsic stability of the molecule
and validate the stability indicating power of the analytical procedures used.
Stress tests are usually considered unnecessary for herbal drugs and herbal drug preparations.
For an active substance the following approaches may be used:
a) When an active substance is described in an official pharmacopoeial monograph
(European Pharmacopoeia or the Pharmacopoeia of a European Union Member State)
and fully meets its requirements no data are required on the degradation products if
they are named under the headings “purity test” and / or “section on impurities”.
b) For active substances not described in an official pharmacopoeial monograph, there are
two options:
- When available, it is acceptable to provide the relevant data published in the
literature to support the proposed degradation pathways;
The stability studies should be conducted on the active substance packaged in a container
closure system that is the same as or simulates the packaging proposed for storage and
distribution.
2.1.5 Specification
Stability studies should include testing of those attributes of the active substance that are
susceptible to change during storage and are likely to influence quality, safety and/or efficacy.
The testing should cover, as appropriate, the physical, chemical, biological, and
microbiological attributes. Validated stability-indicating analytical procedures should be
applied.
Acceptance criteria are numerical limits, ranges and other criteria for the specific tests
described and should include individual and total upper limits for impurities and degradation
products. The justification of individual and total upper limits for degradation products should
be based on safety and/or efficacy considerations. For active substances described in an
official pharmacopoeial monograph (European Pharmacopoeia or the Pharmacopoeia of a
For long-term studies, frequency of testing should be sufficient to establish the stability profile
of the active substance. The frequency of testing at the long term storage condition should
normally be every 3 months over the first year, every 6 months over the second year, and
annually thereafter through the proposed re-test period.
At the accelerated storage condition, a minimum of three points, including the initial and final
time points (e.g., 0, 3, and 6 months), from a 6-month study is recommended. Where an
expectation (based on development experience) exists that results from accelerated studies are
likely to approach significant change criteria, increased testing should be conducted either by
adding samples at the final time point or by including a fourth time point in the study design.
When testing at the intermediate storage condition is called for as a result of significant
change at the accelerated storage condition, a minimum of four time points, including the
initial and final time points (e.g., 0, 6, 9, 12 months), from a 12-month study is recommended.
For herbal drugs and herbal drug preparations on which the applicant in the possession of
historical batch data, the testing frequency may be reduced if justified by the applicant.
In general, an active substance should be evaluated under storage conditions (with appropriate
tolerances) that test its thermal stability and, if applicable, its sensitivity to moisture. The
storage conditions and the lengths of studies chosen should be sufficient to cover storage,
shipment, and subsequent use.
The long term testing for both options a and b should cover a minimum of 6 months’ duration
at the time of submission and should be continued for a period of time sufficient to cover the
proposed re-test period. Additional data accumulated during the assessment period of the
registration application should be submitted to the authorities if requested. Data from the
accelerated storage condition and, if appropriate, from the intermediate storage condition can
be used to evaluate the effect of short-term excursions outside the label storage conditions
(such as might occur during shipping).
Long term, accelerated, and, where appropriate, intermediate storage conditions for active
substances are detailed in the sections below. The general case applies if a subsequent section
does not specifically cover the active substance. Alternative storage conditions can be used if
justified.
* It is up to the applicant to decide whether long term stability studies are performed at
25° C ± 2° C/60 % RH ± 5 % RH or 30° C ± 2°C/65% RH ± 5% RH. In the latter case,
no additional data under intermediate conditions will have to be generated.
** For herbal drugs and herbal drug preparations, testing at the accelerated storage
condition or at the intermediate storage condition may be omitted if justified by the
applicant and if the storage conditions below 25° C are clearly labelled on the product.
When “significant change” occurs at any time during 6 months’ testing at the accelerated
storage condition, additional testing at the intermediate storage condition should be conducted
and evaluated against significant change criteria. Testing at the intermediate storage condition
should include all tests, unless otherwise justified. The initial application should include a
minimum of 6 months’ data from a 12-months study at the intermediate storage condition.
“Significant change” for an active substance is defined as failure to meet its specification.
Data from refrigerated storage should be assessed according to the evaluation section of this
guideline, except where explicitly noted below.
If significant change occurs between 3 and 6 months’ testing at the accelerated storage
condition, the proposed re-test period should be based on the real time data available at the
long term storage condition.
If significant change occurs within the first 3 months’ testing at the accelerated storage
condition, a discussion should be provided to address the effect of short term excursions
outside the label storage condition, e.g., during shipping or handling. This discussion can be
supported, if appropriate, by further testing on a single batch of the active substance for a
period shorter than 3 months but with more frequent testing than usual. It is considered
unnecessary to continue to test an active substance through 6 months when a significant
change has occurred within the first 3 months.
For active substances intended for storage in a freezer, the re-test period should be based on
the real time data obtained at the long-term storage condition. In the absence of an
accelerated storage condition for active substances intended to be stored in a freezer, testing
on a single batch at an elevated temperature (e.g., 5° C ± 3° C or 25° C ± 2° C) for an
appropriate time period should be conducted. Such a study will address the effect of short
term excursions outside the proposed label storage condition, e.g., during shipping or
handling.
Active substances intended for storage below –20° C should be treated on a case-by-case
basis.
When available long term stability data on primary batches do not cover the proposed re-test
period granted at the time of approval, a commitment should be made to continue the stability
studies post approval in order to firmly establish the re-test period.
Where the submission includes long-term stability data on three production batches covering
the proposed re-test period, a post approval commitment is considered unnecessary.
Otherwise, one of the following commitments should be made:
1. If the submission includes data from stability studies on at least three production
batches, a commitment should be made to continue these studies through the proposed
re-test period.
2. If the submission includes data from stability studies on fewer than three production
batches, a commitment should be made to continue these studies through the proposed
re-test period and to place additional production batches, to a total of at least three, on
long term stability studies through the proposed re-test period.
3. If the submission does not include stability data on production batches, a commitment
should be made to place the first three production batches on long term stability studies
through the proposed re-test period.
The stability protocol used for long-term studies for the stability commitment should be the
same as that for the primary batches, unless otherwise scientifically justified.
2.1.9 Evaluation
The purpose of the stability study is to establish, based on testing a minimum of two or three
batches of the active substance and evaluating the stability information (including, as
appropriate, results of the physical, chemical, biological, and microbiological tests), a re-test
period applicable to all future batches of the active substance manufactured under similar
circumstances. The degree of variability of individual batches affects the confidence that a
2.1.10 Statements/Labelling
The storage conditions (temperature, light, humidity) indicated should refer to the Guideline
on Declaration of Storage Conditions for Medicinal Products in the Product Particulars and
Active Substances (CPMP/QWP/609/96).
The use of terms such as “ambient conditions” or “room temperature” is unacceptable.
2.2.1 General
The design of the formal stability studies for the finished product should be based on
knowledge of the behaviour and properties of the active substance and the dosage form.
Photostability testing should be conducted on at least one primary batch of the finished
product if appropriate. The standard conditions for photostability testing are described in the
At the time of submission data from stability studies should be provided for batches of the
same formulation and dosage form in the container closure system proposed for marketing.
Two options are acceptable:
a) For conventional dosage forms (e.g. immediate release solid dosage forms, solutions)
and when the active substances are known to be stable, stability data on at least two
pilot scale batches are acceptable.
b) For critical dosage forms or when the active substances are known to be unstable,
stability data on three primary batches are to be provided. Two of the three batches
should be of at least pilot scale, the third batch may be smaller.
The manufacturing process used for primary batches should simulate that to be applied to
production batches and should provide product of the same quality and meeting the same
specification as that intended for marketing. Where possible, batches of the finished product
should be manufactured by using different batches of the active substance.
Stability studies should be performed on each individual strength and container size of the
finished product unless bracketing or matrixing is applied.
Other supporting data can be provided.
Stability testing should be conducted on the dosage form packaged in the container closure
system proposed for marketing (including, as appropriate, any secondary packaging and
container label). Any available studies carried out on the product outside its immediate
container or in other packaging materials can form a useful part of the stress testing of the
dosage form or can be considered as supporting information, respectively.
2.2.5 Specification
Stability studies should include testing of those attributes of the finished product that are
susceptible to change during storage and are likely to influence quality, safety and/or efficacy.
The testing should cover, as appropriate, the physical, chemical, biological, and
microbiological attributes, preservative content (e.g. antioxidant, antimicrobial preservative),
and functionality tests (e.g., for a dose delivery system). Analytical procedures should be
fully validated and stability indicating. Whether and to what extent replication should be
performed will depend on the results of validation studies.
Shelf life acceptance criteria should be derived from consideration of all available stability
information. It may be appropriate to have justifiable differences between the shelf life and
release acceptance criteria based on the stability evaluation and the changes observed on
storage. Any differences between the release and shelf life acceptance criteria for
antimicrobial preservative content should be supported by a validated correlation of chemical
content and preservative effectiveness demonstrated during drug development on the product
in its final formulation (except for preservative concentration) intended for marketing. A
single primary stability batch of the finished product should be tested for antimicrobial
preservative effectiveness (in addition to preservative content) at the proposed shelf life for
For long-term studies, frequency of testing should be sufficient to establish the stability profile
of the finished product. The frequency of testing at the long term storage condition should
normally be every 3 months over the first year, every 6 months over the second year, and
annually thereafter through the proposed shelf life.
At the accelerated storage condition, a minimum of three points, including the initial and final
time points (e.g., 0, 3, and 6 months), from a 6-month study is recommended. Where an
expectation (based on development experience) exists that results from accelerated testing are
likely to approach significant change criteria, increased testing should be conducted either by
adding samples at the final time point or by including a fourth time point in the study design.
When testing at the intermediate storage condition is called for as a result of significant
change at the accelerated storage condition, a minimum of four time points, including the
initial and final time points (e.g., 0, 6, 9, 12 months), from a 12-month study is recommended.
For herbal medicinal products on which the applicant in the possession of historical batch
data, the testing frequency may be reduced if justified by the applicant.
Reduced designs, i.e., matrixing or bracketing, where the testing frequency is reduced or
certain factor combinations are not tested at all, can be applied, if justified.
In general, a finished product should be evaluated under storage conditions (with appropriate
tolerances) that test its thermal stability and, if applicable, its sensitivity to moisture or
potential for solvent loss. The storage conditions and the lengths of studies chosen should be
sufficient to cover storage, shipment, and subsequent use.
Stability testing of the finished product after constitution or dilution, if applicable, should be
conducted to provide information for the labelling on the preparation, storage condition, and
in-use period of the constituted or diluted product. This testing should be performed on the
constituted or diluted product through the proposed in-use period on primary batches as part
of the formal stability studies at initial and final time points and, if full shelf life long term
data will not be available before submission, at six months or the last time point for which
data will be available. In general, this testing need not be repeated on commitment batches.
The long term testing should cover a minimum of 6 months’ duration (option a) or 12 months’
duration (option b) at the time of submission and should be continued for a period of time
sufficient to cover the proposed shelf life. Additional data accumulated during the assessment
period of the registration application should be submitted to the authorities if requested. Data
from the accelerated storage condition and, if appropriate, from the intermediate storage
condition can be used to evaluate the effect of short-term excursions outside the label storage
conditions (such as might occur during shipping).
Long term, accelerated, and, where appropriate, intermediate storage conditions for finished
products are detailed in the sections below. The general case applies if a subsequent section
does not specifically cover the finished product. Alternative storage conditions can be used, if
justified.
* It is up to the applicant to decide whether long term stability studies are performed at
25° C ± 2° C/60% RH ± 5% RH or 30° C ± 2° C/65% RH ± 5% RH. In the latter case,
no additional data under intermediate conditions will have to be generated.
When a “significant change" occurs at any time during 6 months'testing at the accelerated
storage condition, additional testing at the intermediate storage condition should be conducted
and evaluated against significant change criteria. The initial application should include a
minimum of 6 months’ data from a 12-month study at the intermediate storage condition.
In general, “significant change” for a finished product is defined as:
1. A 5% change in assay from its initial value; or failure to meet the acceptance criteria for
potency when using biological or immunological procedures;
2. Any degradation product exceeding its acceptance criterion;
3. Failure to meet the acceptance criteria for appearance, physical attributes, and
functionality test (e.g., colour, phase separation, resuspendibility, caking, hardness, dose
delivery per actuation); however, some changes in physical attributes (e.g., softening of
suppositories, melting of creams, partial loss of adhesion for transdermal products) may
be expected under accelerated conditions;
And, as appropriate for the dosage form:
4. Failure to meet the acceptance criterion for pH; or
5. Failure to meet the acceptance criteria for dissolution for 12 dosage units.
Sensitivity to moisture or potential for solvent loss is not a concern for finished products
packaged in impermeable containers that provide a permanent barrier to passage of moisture
or solvent. Thus, stability studies for products stored in impermeable containers can be
conducted under any controlled or ambient humidity condition.
When a significant change other than water loss occurs during the 6 months’ testing at the
accelerated storage condition, additional testing at the intermediate storage condition should
be performed as described under the general case to evaluate the temperature effect at 30° C.
A significant change in water loss alone at the accelerated storage condition does not
necessitate testing at the intermediate storage condition. However, data should be provided to
demonstrate that the finished product will not have significant water loss throughout the
proposed shelf life if stored at 25° C and the reference relative humidity of 40% RH.
A 5% loss in water from its initial value is considered a significant change for a product
packaged in a semi-permeable container after an equivalent of 3 months’ storage at 40°
C/NMT 25% RH. However, for small containers (1 ml or less) or unit-dose products, a water
loss of 5% or more after an equivalent of 3 months’ storage at 40° C/NMT 25% RH may be
appropriate, if justified.
An alternative approach to studying at the reference relative humidity as recommended in the
table above (for either long term or accelerated testing) is performing the stability studies
under higher relative humidity and deriving the water loss at the reference relative humidity
through calculation. This can be achieved by experimentally determining the permeation
coefficient for the container closure system or, as shown in the example below, using the
calculated ratio of water loss rates between the two humidity conditions at the same
temperature. The permeation coefficient for a container closure system can be experimentally
determined by using the worst case scenario (e.g., the most diluted of a series of
concentrations) for the proposed finished product.
Example of an approach for determining water loss:
For a product in a given container closure system, container size, and fill, an appropriate
approach for deriving the water loss rate at the reference relative humidity is to multiply the
water loss rate measured at an alternative relative humidity at the same temperature by a water
loss rate ratio shown in the table below. A linear water loss rate at the alternative relative
humidity over the storage period should be demonstrated.
For example, at a given temperature, e.g., 40° C, the calculated water loss rate during storage
at NMT 25% RH is the water loss rate measured at 75% RH multiplied by 3.0, the
corresponding water loss rate ratio.
Valid water loss rate ratios at relative humidity conditions other than those shown in the table
above can also be used.
For finished products intended for storage in a freezer, the shelf life should be based on the
real time data obtained at the long-term storage condition. In the absence of an accelerated
storage condition for finished products intended to be stored in a freezer, testing on a single
Finished products intended for storage below –20° C should be treated on a case-by-case
basis.
When available long-term stability data on primary batches do not cover the proposed shelf
life granted at the time of approval, a commitment should be made to continue the stability
studies post approval in order to firmly establish the shelf life.
Where the submission includes long-term stability data on three production batches covering
the proposed shelf life, a post approval commitment is considered unnecessary. Otherwise,
one of the following commitments should be made:
1. If the submission includes data from stability studies on at least three production
batches, a commitment should be made to continue the long-term studies through the
proposed shelf life.
2. If the submission includes data from stability studies on fewer than three production
batches, a commitment should be made to continue the long term studies through the
proposed shelf life, and to place additional production batches, to a total of at least
three, on long term stability studies through the proposed shelf life and on accelerated
studies for 6 months.
3. If the submission does not include stability data on production batches, a commitment
should be made to place the first three production batches on long term stability studies
through the proposed shelf life and on accelerated studies for 6 months.
The stability protocol used for studies on commitment batches should be the same as that for
the primary batches, unless otherwise scientifically justified.
Where intermediate testing is called for by a significant change at the accelerated storage
condition for the primary batches, testing on the commitment batches can be conducted at
either the intermediate or the accelerated storage condition. However, if significant change
occurs at the accelerated storage condition on the commitment batches, testing at the
intermediate storage condition should also be conducted.
2.2.9 Evaluation
A systematic approach should be adopted in the presentation and evaluation of the stability
information, which should include, as appropriate, results from the physical, chemical,
biological and microbiological tests, including particular attributes of the dosage form (for
example, dissolution rate for solid oral dosage forms).
The purpose of the stability study is to establish, based on testing a minimum of two or three
batches of the finished product, a shelf life and label storage instructions applicable to all
future batches of the finished product manufactured and packaged under similar
circumstances. The degree of variability of individual batches affects the confidence that a
future production batch will remain within specification throughout its shelf life.
2.2.10 Statements/Labelling
The storage conditions (temperature, light, humidity) indicated should refer to the Guideline
on Declaration of Storage Conditions for Medicinal Products in the Product Particulars and
Active Substances (CPMP/QWP/609/96).
The use of terms such as “ambient conditions” or “room temperature” is unacceptable.
ANNEX I
ANNEX II
Extrapolation of data
If real time data are supported by results from studies conducted under accelerated or
intermediate storage conditions, the re-test period/shelf life may be extended beyond the end
of real time studies. The extrapolated retest period or shelf-life may be up to twice, but should
Significant
change at No
accelerated
condition within
3 months?
Yes
No No
Yes to both
Yes to both
If backed by statistical
analysis and relevant If backed by relevant
Y= up to 2X, but not supporting data: Y = up to supporting data: Y = up
exceeding X + 12 months; 2X, but not exceeding X + to 1.5X, but not
or if refrigerated, 12 months; or if refrigerated, exceeding X + 6 months;
Y = up to 1.5X, but not Y = up to 1.5X, but not or if refrigerated, Y = up
exceeding X + 6 months exceeding X + 6 months to X + 3 months