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Development Process Validation
Process Validation During Clinical Development of Biological Medicinal Products
Siegfr ied Schmitt
Principal Consultant, PAREXEL Consulting
AbstractThe need for process validation is well understood and a regulatory requirement. However, process validation occurs over a lengthy period
of time, and the depth and detail of effort is dependent on many factors during the clinical phases. Biological products are different in many
respects from their chemical counterparts and thus process validation expertise cannot simply be transferred from one to the other. This
article addresses good industry practices in applying process validation efforts that meet regulatory expectations.
KeywordsClinical development, biological products, process validation, industry best practice
Disclosure: The author has no conflicts of interest to declare.
Acknowledgement: The author wishes to thank his PAREXEL Consulting colleagues for their feedback and input on the manuscript: David Chesney, Vice President, Strategic
Compliance; Cecil Nick, Vice President Biotechnology; Ravi S Harapanhalli, Principal Consultant; and Karen Jette, Senior Consultant.
Received: 16 July 2009 Accepted: 20 August 2009
Correspondence: Siegfried Schmitt, PAREXEL Consulting, The Quays, 101–105 Oxford Road, Uxbridge, Middlesex, UB8 1LZ, UK. E: [email protected]
Development of the biopharmaceutical production process begins
immediately after the discovery phase, continues through to
regulatory submission and extends post-approval. From the authorities’
perspective, it is essential that the process is sufficiently validated and
that such evidence is part of the submission for marketing authorisation.
The need for validation is described in the relevant regulations
governing healthcare products. By its very nature, the early phases of
product development result in various changes to the manufacturing
process and associated analytical procedures. Therefore, the question
arises of how validation should be approached from the perspective
of regulatory compliance and industry best practice. Process
validation for biologics is more complex than for chemical drug
products due to the number of process steps and sensitivity to
external variations, e.g. batches of raw materials, working cell banks
and harvest times. The quality of each component of the process,
including raw materials, reagents and excipients, must be controlled.
From Process Development to ValidationProcess DevelopmentDuring process development, data are generated and collected that
can assist in the identification or verification of critical process
parameters and statistical process controls. These data enable the
establishment of process limits and operational process parameters
(specifications). The criticality of each process parameter is determined
by analysing the relationship between the selected operating range,
proven acceptable range, the alarm and failure limits.1
Process ValidationThe US Food and Drug Administration (FDA) draft guidance document,
Guidance for Industry, Process Validation: General Principles and
Practices2 from November 2008 defines process validation as “…the
collection and evaluation of data, from the process design stage
throughout production, which establishes scientific evidence that a
process is capable of consistently delivering quality products” (see
Table 1). Thus, the ‘life-cycle’ approach to process validation begins
with process design, followed by process qualification, performance
qualification and continuing through commercial production.
There are a number of prerequisites that must be met before process
validation can begin (see Table 2). It is essential to understand that some
of these activities can and may overlap (e.g. product characterisation
and assay development), whereas others should be followed
sequentially (e.g. assay validation and process validation; see Figure 1).
Manufacture of Biological InvestigationalMedicinal Products Is Complex Early PhaseManufacture of biological investigational medicinal products (IMPs) is
a highly complex process. Beginning initial production of IMPs is
especially challenging as there are no fixed manufacturing routines.
In addition, IMPs are typically produced on a small scale on a
campaign basis or along with a multitude of other products, which in
turn increases the risk of product cross-contamination and potential
mistakes due to mix-ups. This means there is a need for robust
quality systems that can cope with the flexible nature of the IMP
production process.
The inherent complexity of manufacturing biological products and
magnitude of the challenge becomes apparent as development of the
manufacturing process progresses. This complexity arises from limited
and incomplete knowledge about the biological IMPs and, most
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Development Process Validation
D R U G : D E V E L O P M E N T76
importantly, the impact various process steps have on its quality
attributes, which may affect toxicity and potency. Product quality (purity
and structural integrity) can be very sensitive to even minor variations in
the process parameters. Such variations can be caused, for example, by
changes in downstream purification equipment, such as columns. As the
process is developed and scaled up, critical process parameters need to
be identified and an adequate control strategy needs to be built around
them. Separating the critical process parameters into scale-dependent
and scale-independent parameters provides a scientific basis for a
process scale-up. Hence, scale-up of biological IMPs is no trivial activity.
Moreover, many process changes, including process scale-up, require
prior approval and scrutiny from regulatory agencies.
Typically, the manufacturing of biological IMPs results in limited
product quantities, which represent significant financial value. This
limits the number and type of experiments that can be performed as
part of process development. This also has a direct impact on the
quantity of materials (including both product and impurities) available
for concurrent analytical method development. In these cases
manufacturing processes and information transfer are challenging.
Initially more is documented on paper; later computer systems are
typically set up to capture process data.
Finally regulatory requirements are extensive. For example,
the Clinical Trials Directive (www.ec.europa.eu/enterprise/
pharmaceuticals/eudralex/vol10_en.htm) and Good Manufacturing
Practice (GMP) Directive (www. ec.europa.eu/enterprise/
pharmaceuticals/eudralex/vol4_en.htm) in the EU impose many
obligations on the manufacturer of biological IMPs. Similarly, the US
FDA requires progressive application of GMPs and chemistry,
manufacturing and controls (CMC) documentation as the
investigational new drug application proceeds with biologic
development. The FDA guidance Current Good Manufacturing
Practice for Phase 1 Investigational Drugs – July 2008 describes the
expectations for GMPs during phase I investigational new drug stages.
It is expected that 21 CFR210/211 requirements are applied during
phase II and III leading up to the approval of a new drug application or
a biological licence application (BLA) and beyond.
The US current GMP (cGMP) requirement was added to the Federal
Food, Drug and Cosmetic Act (FDC Act) in 1962, and the term ‘current’
in ‘current good manufacturing practice’ is both feasible and valuable
in assuring drug quality. In applying this concept to process validation
for the manufacture of clinical trial materials, it is clearly not feasible
to validate a process that is not robust and still under development.
This is because validation is intended to show repeatability. If the
product is not being manufactured in a repeatable fashion,
validation is not ‘feasible’ and should not be expected. This view is
consistent with the FDA’s 2008 guideline on the manufacture of
investigational drugs (www.fda.gov/downloads/Drugs/Guidance
ComplianceRegulatoryInformation/Guidances/UCM070273.pdf).
At early clinical stages, where a single batch of drug product may be
produced, and where significant formulation and processing changes
may make batch replication difficult or inexact, only limited process
validation may be possible. In such cases limited validation, especially
for such critical processes as sterilisation, should be derived to the
extent possible from product and process analogues. In addition, data
obtained from extensive in-process controls and intensive product
testing may be used to demonstrate that the instant run yielded a
finished product meeting all of its specifications and quality
characteristics. It is expected that more comprehensive process
validation will be conducted as additional uniform batches are made
under replicated conditions. On the other hand, it is clearly
possible to qualify fixed resources, such as manufacturing equipment
and facility support systems (water, gases, vacuum, etc.) and
manufacturing-associated computer systems. Therefore, it is
expected that equipment qualification (as distinct from process
validation) will be completed sooner, in the early phases of biological
IMP development. Thus, full process validation can only take place
once manufacturing process development is complete. However, the
knowledge accrued during process development will contribute to final
validation activities conducted before or during phase III.
In the US, biological medicinal products can be approved under the FDC
Act as a new drug application or under the Public Health Service Act as
a BLA depending on the nature of the biologic. While the Center for
Drug Evaluation and Research provides for completion of process
validation activities prior to commercialisation, the Center for Biologic
Evaluation and Research requires that the biologic manufacturing
process is validated during phase III and prior to the submission of a
BLA application. In view of the structural complexity of biologic
medicinal products, which are often intimately linked to the
manufacturing processes, it is recommended that the process
validation be completed during phase III studies.
Table 1: Key Regulations and Guidance
US Code of Federal Regulations 21 CFR Parts 210 and 211
FDA Guideline of General Principles of Process Validation, May 1987:
www.fda.gov/cder/guidance/pv.htm
FDA Draft Guidance for Industry Process Validation: General Principles and
Practices, November 2008: www.fda.gov/cvm/Guidance/guide196.pdf
FDA Compliance Program Guidance Manual Chapter – 45, Inspection of Biological
Drug Products (CBER) 7345.848: www.fda.gov/cber/cpg/7345848.pdf
FDA Sec. 490.100 Process Validation Requirements for Drug Products and Active
Pharmaceutical Ingredients Subject to Pre-Market Approval (CPG 7132c.08):
www.fda.gov/ora/compliance_ref/cpg/cpgdrg/cpg490-100.html
PIC/S Recommendation on the Validation of Aseptic Processes, PI 007-4,
7 February 2009: www.picscheme.org
EudraLex – Volume 1 – Pharmaceutical Legislation, Medicinal Products for Human
Use: www.ec.europa.eu/enterprise/pharmaceuticals/eudralex/vol1_en.htm
EudraLex – Volume 4, Good manufacturing practice (GMP) Guidelines & Annexes:
www.ec.europa.eu/enterprise/pharmaceuticals/eudralex/vol4_en.htm
EudraLex – Volume 10, Clinical trials guidelines: www.ec.europa.eu/enterprise/
pharmaceuticals/eudralex/vol10_en.htm
Guideline for the Determination of Residual Moisture in Dried Biological Products,
January 1990: www.fda.gov/ohrms/dockets/dockets/05d0047/05d-0047-bkg0001-
Tab-11.pdf
Guidance for Industry for the Submission Documentation for Sterilization Process
Validation in Applications for Human and Veterinary Drug Products, November 1994
Table 2: Prerequisites for Process Validation
Process development
Facility qualification
Equipment and utilities qualification
Raw materials and excipients qualification
Analytical method validation
Cleaning method validation
Computerised systems validation
Training
Standard operating procedures (at least in draft)
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Process Validation During Clinical Development of Biological Medicinal Products
D R U G : D E V E L O P M E N T 77
Some critical processes will need to be validated even at phase I.
These include:
• aseptic processing, where possible;
• viral clearance validation should be no less rigorous than for
products authorised for marketing (www.ec.europa.eu/enterprise/
pharmaceuticals/eudralex/vol-4/pdfs-en/an13final_24-02-05.pdf);
• homogeneity issues; and
• removal of critical impurities (highly toxic, immunogenic, mutagenic,
prions, etc.) to levels below the limit of detection, where relevant.
Although for phase I full validation will not be required there are initial
steps towards validation that will need to be taken, such as
qualification of equipment and of analytical methods. The FDA
guidance Sterile Drug Products Produced by Aseptic Processing –
Current Good Manufacturing Practice (www.fda.gov/ohrms/dockets/
ac/05/briefing/2005-4136b1_04_Sterile%20Drug%20Products.pdf)
provides for validation requirements for aseptic processes and this is
expected to be completed as soon as practicable during the initial
stages of the new drug investigation.
Late PhaseLate phase is generally defined as post-proof-of-concept, which is close
to the end of phase II and the beginning of phase III. The following is a
recommended outline of activities related to process validation:
• end of phase II/phase III: consider whether any critical parts of the
process should be validated and justify omissions;
• prior to medical administrive activities/new drug application/BLA:
• completion of validation;
• revalidation following scale-up;
• manufacture of at least three qualification batches.
Process validation cannot take place until the equipment, facilities
and services have been qualified and standard operating procedures
prepared. Furthermore, analytical methods will need to have been
validated before process validation is applied for. The critical steps
that require special attention as part of the validation process will
need to be identified.
Establishing appropriate validation acceptance criteria (VAC) is one of
the greatest challenges in the development of a commercial
biological IMP manufacturing process. Manufacturers with VACs that
are too broad will not be able to demonste adequate process control.
However, if the manufacturer sets its VAC too tight this can result in
failed validation runs, even though the process may be performing
adequately.3
In addition, there is a need to understand potential impurities and have
validated methods available to detect these. Target limits will need to be
set and justified for in-process control, release and end of shelf-life
testing. These limits should be based on data amassed during biological
IMP production and process development as well as trend analyses,
pharmacopoeial and other regulatory requirements and precedence,
including assessment of safety.
The following issues are often encountered during inspections
pertaining to process validation and are often quoted in inspection
reports, such as 483 observations, by investigators:
• lack of documented procedures and documented validation results;
• sampling or sample preparation step contributing to overall error;
• accessories and materials used for equipment qualification
not qualified;
• lack of computer system validation (this is in addition to the
software and hardware qualification requirements);
• qualification and validation are carried out at just one particular
point in time; and
• adaptation of acceptance criteria for qualification of new system
without adequate justification.
The Process and Its ValidationValidation requirements differ in terms of the specific manufacturing
process involved and whether the process occurs upstream,
downstream or fill and finish.
UpstreamFermentation represents the critical component of the upstream
process and is typically scaled-up several times, which may impact
on biological IMP quality, safety and/or efficacy. Thus, to support the
scale-up activities, a comprehensive physico-chemical and biological
testing programme will be required. If differences are detected,
supporting non-clinical and clinical data may be required for late-
phase changes. For phase I, the facilities and equipment will need to
have been qualified. Trend analyses will continue with full validation
being conducted on at least three consecutive batches. Upstream
validation will need to justify in-process controls. For example, this
can be performed by testing the process at the extremities of the
limits. Criteria for batch rejection will need to be established as well
as criteria for termination of fermentation based on, for example, the
maximum generation number, continuous fermentation cultivation
period and criteria for premature termination.
DownstreamDownstream processing involves purification and such critically
important processes as virus clearance, which are required to be
validated even at phase I. During later development phases it
will also be necessary to validate removal of any critical or
toxic impurities. By medical administrative activities/new drug
application/BLA submission, validation will need to address issues
such as: column loading capacity, regeneration, period of use,
sanitisation, potential for leaching, storage, cleaning and sanitisation.
Cleaning/washing and sanitisation (percentage of ethanol or sodium
Figure 1: Development and Validation Timelines
Activity
Clone selection
Cell bank characterisation
Process development
Scale-up
Technical feasibility
Economic viability
Assay development
Assay validation
Product characterisation
Process validation
Documentation
Regulatory support
Pre-clinical Phase I Phase II Phase III
Preliminary work Significant effort Extensive activity
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Development Process Validation
D R U G : D E V E L O P M E N T78
hydroxide) of the column packing will be needed to be both
established and verified. Small-scale spiking studies may need to be
performed on DNA, host-cell proteins and media contaminants, such
as antibiotics, if used.
Fill and FinishProteins are generally labile, so terminal sterilisation is usually not
possible and reliance on aseptic processing is required. This is a
critical issue that needs to be validated even at phase I. Validation of
aseptic processes presents special problems when the batch size is
small; in these cases the number of units filled may be the maximum
number filled in production. However, if practicable and otherwise
consistent with simulating the process a larger number of units
should be filled to provide greater confidence in the results obtained.
During biological IMP production, filling and sealing is often a manual
or semi-automated operation presenting great challenges to sterility,
so enhanced attention should be given to operator training and
validating the aseptic technique of individual operators.
Spray drying and lyophilisation are two common processes in the
finishing of dosage forms. Spray drying involves continuous
atomisation of the feed solution into a hot drying gas, most commonly
air or nitrogen. The fine droplets resulting from the atomisation of the
feed solution are immediately exposed to the drying gas leading to
supersaturation and resulting in the formation of ultra-fine particles,
typically below 5μ and with a tight particle size distribution, which are
collected via a cyclone. The end product must comply with precise
quality standards regarding particle size, distribution, residual
moisture content, bulk density and morphology.
It is recognised that there is complex technology associated with the
manufacture and control of a lyophilised pharmaceutical dosage
forms. Some of the important aspects of these operations include the
formulation of solutions, filling of vials and validation of the filling
operation, sterilisation and engineering aspects of the lyophiliser and
testing of the end product.
Freeze-drying (lyophilisation) has successfully been used for the
preservation and storage of many vaccines, microbial cultures and
other labile biological products. Certain biological preparations are
lyophilised in order to maintain integrity, potency and other properties
of the product, when for that particular product other methods of
preservation, such as freezing alone or addition of a preservative,
have not been found to provide sufficient stability. Residual moisture
has been the term used to describe the low level of surface water,
usually from less than 1–5%, remaining in a freeze-dried vaccine or
other biological product after the bulk of the aqueous solvent has
been removed during the freeze-drying (vacuum sublimation)
process. Examples of freeze-dried biological products include
antihemophilic factor (human), measles virus vaccine live,
streptokinase, alfa interferon, typhoid vaccine, meningococcal
polysaccharide vaccine groups A and C combined and wasp venom
allergenic extract.
Levels of residual moisture should be sufficiently low so that, where
applicable, the viability, immunologic potency and integrity of the
product are not compromised over time. However, levels of residual
moisture for certain products should not be so low that the properties
of the product, i.e. viability, are compromised by overdrying.4
Overdrying may cause living cells to lose viability, cause the tertiary
molecular structure of complex proteins to be altered with
subsequent loss of activity, or remove monolayers of water from
active sites on molecules that can then react with traces of
oxygen and thus degrade. Each product needs to be evaluated on a
case-by-case basis to determine the optimum residual moisture level.
Therefore, the approach to process validation should take into
consideration developmental data on residual moisture content
needed for optimal stability of lyophilised products. The industry
guidance Guideline for the Determination of Residual Moisture in
Dried Biological Products (www.fda.gov/ohrms/dockets/dockets/
05d0047/05d-0047-bkg0001-Tab-11.pdf) provides additional details.
Recent inspections have disclosed potency and sterility problems
associated with the manufacture and control of lyophilised products.
Some of the common inspectional observations pertaining to freeze
drying of biopharmaceuticals include the following issues:
• failure to adequately ensure that when the results of a process
cannot be fully verified by subsequent inspection and test, that the
process shall be validated with a high degree of assurance and
approved according to established procedure;
• failure to establish acceptance criteria for validation of the
freeze-drying process for the manufacturing of a product prior to
initiating the validation;
• assessing or varying different parameters but not evaluating the
parameters used during the routine freeze-drying process;
• validation study not representing a typical production batch size;
• unable to produce process validation documentation including
installation qualification records for the freezer or lyophiliser;
• failure to establish and maintain procedures for implementing
corrective and preventive actions that include requirements for
analysing sources of quality data to identify existing and potential
causes of non-conforming product, or other quality problems;
• failure to conduct appropriate validation studies for critical
processes such as cleaning procedures for equipment and
inactivation.
SummaryValidation is a progressive process resulting in continuous collation
of data, refinement of critical quality attributes and transformation
of information into knowledge. For biopharmaceutical products in
particular, some highly critical process parameters will have to be
established early on in the product development life-cycle, possibly
as soon as phase I. It is essential to integrate activities for process
development and optimisation, collation of evidence for regulatory
filing and operational cost management. This helps to avoid
duplication of effort and assists in achieving the right balance
between quality, cost and operational excellence. In order to
achieve such an outcome, companies will have to employ modern
tools and technology, paired with the experience and expertise of a
variety of subject matter experts, including process engineers,
industrial pharmacists, analytical chemists, microbiologists,
statisticians, manufacturing experts and quality assurance
personnel. It is a team effort. n
1. Fetterolf DM, BioPharm International, 2007;20(12).
2. Guidance for Industry, Process Validation: General
Principles and Practices, 2008. Available at:
www.fda.gov/downloads/Drugs/GuidanceCompliance
RegulatoryIn...n/Guidances/UCM070336.pdf
3. Burdick R, BioPharm International, 2007;20(6).
4. Grieff D, Rightsel W, Applied Microbiology, 1968;16:835–40.
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