ICH E6-R3 GCP-Principles Draft 2021 0419
ICH E6-R3 GCP-Principles Draft 2021 0419
ICH E6-R3 GCP-Principles Draft 2021 0419
The International Council for Harmonisation (ICH) is committed to developing timely technical
requirements for pharmaceuticals for human use in a manner that is responsive to the needs of the
global community. ICH is committed to stakeholder engagement and transparency in the development
of its guidelines.
ICH E6 Good Clinical Practice (GCP) Guideline is widely used by clinical trial researchers beyond the
membership and regional representation of ICH itself and has a significant impact on trial participants
and patients. Acknowledging the wide and substantial impact of ICH E6, the ICH Management
Committee is making available a draft, work-in-progress version of the updated principles that are
currently under development by the ICH E6(R3) Expert Working Group (EWG). The principles are
interdependent and should be considered in their totality to assure ethical trial conduct, participant
safety, and reliable results of clinical trials.
The renovation of ICH E6(R2) will set out principles which will be aligned with the principles in ICH
E8(R1) Revision of General Considerations for Clinical Studies. ICH E8(R1) includes a framework for
designing quality into clinical trials, stakeholder engagement, trial design, proportionate trial
management and focus on factors critical to the quality of trials. When complete, ICH E6(R3) will be
composed of an overarching principles document (the document of which a draft is now made public),
Annex 1 (addressing interventional clinical trials), and Annex 2 (providing any needed additional
considerations for non-traditional interventional clinical trials). The overarching principles document
and Annex 1 will replace the current ICH E6(R2).
Although the EWG’s work is continuing and the group is still progressing towards Step 2 of the ICH
guidance development process (https://ich.org/page/formal-ich-procedure), the ICH Management
Committee decided that sharing the draft version of the principles would facilitate transparency and
common understanding. Although public comments are not requested at this time, once the updated
ICH E6 Guideline achieves Step 2 of the ICH guidance development process, public input will be invited
and considered. Step 2 will involve simultaneous publication of both the draft principles and Annex 1,
along with an introduction and a glossary. Public comment will be invited at that point since the
principles need to be seen and commented on alongside the details in Annex 1.
The ICH E6(R3) EWG is organizing a web conference to present the current draft of the GCP principles
as a work in progress. Additionally, the general ICH process will be presented with a focus on the ICH
E6(R3) development process.
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ICH E6 Principles
(Draft Version: March 2021)
Clinical trials are a fundamental part of clinical research that support the development of new
medicines or uses of existing medicines. Well designed and conducted clinical trials help answer key
questions in health care and drug development. Their results are essential for evidence-based
healthcare decisions. Trials with inadequate design and/or poorly conducted trials may place
participant safety at risk and yield inadequate or unreliable evidence. They waste resources and the
efforts and time of investigators and participants.
The principles of GCP are designed to be flexible and applicable to a broad range of clinical trials. This
guideline, along with ICH E8, encourages thoughtful consideration and planning to address specific
and potentially unique aspects of an individual clinical trial. This includes evaluation of trial
characteristics, such as the design elements, the investigational product being evaluated, the medical
condition being addressed, characteristics of the participants, the setting in which the clinical trial is
being conducted, and the type of data being collected. Careful consideration of factors relevant to
ensuring trial quality is needed for each clinical trial.
The principles are intended to support improved and more efficient approaches to trial design and
conduct. For example, innovative digital health technologies may expand the possible approaches to
trial conduct. Such technologies can be incorporated in existing healthcare infrastructures and enable
the use of a variety of relevant data sources in clinical trials. This will aid in keeping clinical trial conduct
in line with advancing science and technological developments. The use of technology in the conduct
of clinical trials should be adapted to fit the participant characteristics and the particular trial design.
The use of innovative technologies may help enable those designing and conducting a trial to include
relevant patient populations. This guideline is intended to be media neutral to enable the use of
different technologies for the purposes of documentation.
Clinical trial designs that bring the trial to participants and their communities may improve the
representativeness of the participant population and enable wider participation. The process of
building quality into the design of the trial may be supported by participation of those directly
involved. These may include a broad range of stakeholders, including patients and treating physicians.
Their input can increase the likelihood of meaningful trial outcomes, which are relevant to both trial
participants and future patients. This input will also guide decisions on the feasibility of data collection
and assure that participation in the trial does not become unduly burdensome for those involved.
Clinical trials should be designed to protect the rights, safety and well-being of participants and assure
the reliability of results. Clinical trial designs and processes should be proportionate to the risks
inherent in the trial and the importance of the data being collected. Trial designs and processes should
be evaluated to minimize unnecessary complexity and burden.
The following overarching principles provide a flexible framework for clinical trial conduct. They are
structured to provide guidance throughout the lifecycle of the clinical trial. These principles are
applicable to trials involving human participants, i.e., healthy volunteers or patients. The principles
are interdependent and should be considered in their totality to assure ethical trial conduct and
reliable results.
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1- Clinical trials should be conducted in accordance with the ethical principles that have their
origin in the Declaration of Helsinki and that are consistent with good clinical practice (GCP)
and applicable regulatory requirement(s).
2- Clinical trials should be designed and conducted in ways that ensure the rights, safety, and
well-being of participants.
2.1 The rights, safety, and well-being of the participants are the most important
considerations, and should prevail over interests of science and society.
2.2 The safety of the participants should be reviewed periodically, as new safety
information becomes available which could have an impact on the participant or the
conduct of the trial.
2.3 Foreseeable risks and inconveniences should be weighed against the anticipated
benefits for the individual participants and society. A trial should be initiated and
continued only if the anticipated benefits justify the risks.
2.4 When appropriate, the participant selection process should be representative of the
anticipated population who are likely to use the medicinal product in future clinical
practice. When designing a clinical trial, the scientific goal and purpose should be
carefully considered so as not to unnecessarily exclude particular participant
populations.
2.5 A qualified physician or, when appropriate, a qualified dentist, should have the overall
responsibility for the medical care given to, and medical decisions made on behalf of,
participants; however, the practical interactions and the delivery of medical care and
decisions can be carried out by appropriately qualified health care professionals in
accordance with local regulations.
2.6 The confidentiality of information that could identify participants should be protected
in accordance with applicable privacy and data protection regulations.
3- Informed consent is an integral feature of the ethical conduct of a trial. Clinical trial
participation should be voluntary and based on a consent process that ensures participants
are well-informed.
3.1 Freely given informed consent should be obtained and documented from every
participant prior to clinical trial participation. For participants unable to provide
informed consent, their legally authorized representative should provide consent
prior to clinical trial participation.
3.2 The process and information provided should be designed to achieve the primary
objective of enabling trial participants to make an informed decision on whether or
not to participate in the trial. The informed consent process should take into
consideration relevant aspects of the trial such as characteristics of the participants,
the trial design, anticipated benefit and risk of medical intervention(s), setting and
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context in which the trial will be conducted (e.g., trials in emergency situations), and
the potential use of technology to inform participants and obtain informed consent.
4.1 A trial should always be conducted in compliance with the protocol that receives prior
IRB/IEC approval/favourable opinion.
4.2 Periodic review of the trial by the IRB/IEC should also be conducted as appropriate.
5- Clinical trials should be scientifically sound for their intended purpose, and based on robust
and current scientific knowledge and approaches.
5.2 Clinical trials should be scientifically sound and reflect the state of knowledge and
experience with the investigational product(s); including if applicable, the condition
to be treated, diagnosed, or prevented; the current understanding of the underlying
biological mechanism (of both the condition and the treatment); and the population
for which the investigational product is intended.
5.3 There should be periodic review of current scientific knowledge and approaches to
determine whether adjustments to the trial are needed, since new or unanticipated
information may arise once the trial has begun.
6.1 Individuals with different expertise and training are needed across all phases of a
clinical trial, such as physicians, scientists, ethicists, technology experts, and
statisticians. Individuals involved in a trial should be qualified by education, training,
and experience to perform their respective task(s).
7- Quality should be built into the scientific and operational design and conduct of clinical
trials.
7.1 Quality of a clinical trial is considered in this document as fit for purpose. The quality
and amount of the information generated during a clinical trial should be sufficient to
support good decision making.
7.2 Factors critical to the quality of the trial should be identified. These factors are
attributes of a trial which are fundamental to the protection of participants, the
reliability and interpretability of the trial results, and the decisions made based on
those trial results. These quality factors are critical because, if they were to be
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undermined by errors of design or conduct, the ethical basis of the trial and reliability
of results could also be undermined.
7.3 Quality by design in clinical trial sets out to ensure that the quality of a trial is driven
proactively by designing quality into the study protocol and processes. This may
involve the use of a prospective, multidisciplinary approach to promote the quality of
protocol and process design, and clear communication of how this will be achieved.
Quality by design approaches should be applied across the clinical trial and supporting
processes.
7.4 Strategies should be implemented to avoid, detect, and address serious non-
compliance with GCP and prevent recurrence.
8- Clinical trial processes, measures, and approaches should be proportionate to the risks to
participants and to the reliability of trial results.
8.1 Trial processes should be proportionate to the risks inherent in the trial and the
importance of the information collected. Risks in this context include risks to the
rights, safety and well-being of trial participants, as well as risks to the reliability of
the trial results.
8.2 Risks beyond those of standard medical care should be the focus of considerations;
however, the risks relating to investigational products which have a marketing
authorisation used in the clinical trial context may differ from the usual care of
patients and should be taken into consideration.
8.3 The quality factors should be prioritized at the time of the trial design to identify those
that are critical to the trial.
8.4 Risks which have an impact on the quality factors considered critical to the trial should
be managed.
9- Clinical trials should be described in a clear, concise, and operationally feasible protocol.
9.2 The scientific objectives of any trial should be clear and explicitly stated in the
protocol.
9.3 Trial processes should be operationally feasible and avoid unnecessary complexity,
procedures, and data collection. Trial processes should support the study key
objectives.
9.4 The clinical trial protocol as well as the plans or documents for the protocol execution
(e.g., statistical analysis plan, data monitoring plan) should be clear, concise, and
operationally feasible.
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10.1 The quality and amount of the information 1 generated in a clinical trial should be
sufficient to provide confidence in the trial’s results and support good decision
making.
10.2 Systems and processes that help ensure the quality of the information generated from
the clinical trial should be implemented in a way that is proportionate to the risks to
participants and the reliability of trial results.
10.3 Tools that aid in data capture, management, and analyses should be fit for purpose,
should capture the information required by the protocol, and should conform to
principles that ensure reliable results.
10.4 Digital systems used for clinical trial purposes should consider the factors critical to
their quality in their design and be fit for purpose. To this end, validation of systems,
data protection, information technology (IT) security and user management are
important elements that should be addressed.
10.5 Clinical trials should incorporate efficient and well-controlled processes for managing
information through appropriate management of data integrity, traceability, and
protection of personal information, thereby allowing the accurate reporting,
interpretation, and verification of the clinical trial-related information.
10.8 The principles in this section for trial information and documentation apply
irrespective of the type of media used.
11- Roles, tasks and responsibilities in clinical trials should be clear and documented
appropriately.
11.1 The sponsor and investigator may delegate some or all of their tasks but retain overall
responsibility for the quality and integrity of trial conduct and the safety of
participants.
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For the purpose of this guideline, the term “information” reflects meaningful organization and processing of data and
documentation and “data” reflects measurement and assessment of variable parameters relevant to specific outcomes.
The “results” are a composition of organized and fit-for-purpose information.
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11.2 Agreements should clearly define the roles, tasks and responsibilities for the clinical
trial and be documented appropriately. Where tasks have been delegated or
contracted to third parties, the responsibility is retained by the sponsor or investigator
who should maintain appropriate oversight of these tasks.
12- Investigational products used in a clinical trial should be manufactured in accordance with
applicable Good Manufacturing Practice (GMP) standards and be stored, shipped, and
handled in accordance with the product specifications and the trial protocol.
12.2 Measures should be in place to ensure that the investigational product provided to
trial participants retains its quality.
12.3 Investigational products should be used in accordance with the protocol and relevant
study documents.