ICH E6(R3) Key Sections | GCP Guideline Quick Reference | GCP Resources

ICH E6(R3) Structure Overview

ICH E6(R3), with Step 4 adoption on 06 January 2025, represents the most significant revision to GCP guidelines since 1996. The Step 2 draft was released for public consultation in May 2023. This reference provides a quick navigation guide to the restructured document.

Document Architecture

Component	Purpose	Applicability
Overarching Principles	Foundational GCP principles	All clinical trials
Annex 1	Detailed requirements for interventional IMP trials	Interventional medicinal product trials
Annex 2	Additional considerations for non-traditional approaches	Decentralized trials, digital technologies, pragmatic trials

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Key Points:

Establishes scope applicable to interventional clinical trials of investigational medicinal products
Emphasizes human participant protection and data reliability
Introduces proportionate, risk-based approaches

Section 2: Principles of ICH E6(R3)

The guideline articulates 11 overarching principles that provide a flexible framework for clinical trial conduct throughout the trial life cycle. These principles are interdependent and should be considered in their totality to assure ethical trial conduct and reliable results.

Principle	Title	Focus
Principle 1	Ethical Conduct and Participant Protection	Clinical trials should be conducted in accordance with ethical principles from the Declaration of Helsinki, consistent with GCP and applicable regulatory requirements. Rights, safety, and well-being of participants are paramount.
Principle 2	Informed Consent	Informed consent is integral to ethical trial conduct. Participation should be voluntary, based on a consent process ensuring participants are well-informed.
Principle 3	IRB/IEC Review	Clinical trials should be subject to independent review by an IRB/IEC with documented prior approval before trial initiation.
Principle 4	Scientific Soundness	Clinical trials should be scientifically sound for their intended purpose, based on adequate and current scientific knowledge and approaches.
Principle 5	Qualified Individuals	Clinical trials should be designed and conducted by individuals qualified by education, training, and experience.
Principle 6	Quality by Design	Quality should be built into the scientific and operational design and conduct of clinical trials, with focus on factors critical to quality.
Principle 7	Proportionate Risk-Based Approach	Trial processes, measures, and approaches should be proportionate to risks to participants and importance of data collected, avoiding unnecessary burden.
Principle 8	Protocol Requirements	Clinical trials should be described in a clear, concise, scientifically sound, and operationally feasible protocol.
Principle 9	Reliable Results	Clinical trials should generate reliable results with appropriate data systems, record management, and transparency through registration and results posting.
Principle 10	Roles and Responsibilities	Roles and responsibilities in clinical trials should be clear and documented appropriately, with sponsors and investigators retaining overall responsibility even when activities are delegated.
Principle 11	Investigational Product Management	Investigational products should be manufactured in accordance with applicable GMP standards and managed according to product specifications and trial protocol.

Key E6(R3) Enhancements:

Principles 6 and 7 introduce the risk-proportionate, quality-by-design approach central to E6(R3)
Principle 9 emphasizes data reliability, computerized systems validation, and trial transparency
Principle 10 addresses the complex ecosystem of sponsors, investigators, and service providers with clear accountability

Section 3: Quality Management

Critical Concepts:

Critical to Quality (CtQ) Factors: Elements essential to participant protection and data reliability
Risk-Based Quality Management: Prospective identification, assessment, and control of risks
Proportionality: Activities scaled to risk level of the trial

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

Topic	Key Content
Responsibilities	Protocol review, continuing review, safety monitoring
Composition	Qualified membership requirements
Documentation	Records of meetings, decisions, member qualifications

A1.2 Investigator

Topic	Key Content
Qualifications	Education, training, experience requirements
Resources	Adequate facilities, equipment, staff
Medical care	Participant medical decisions
Informed consent	Process and documentation
Protocol compliance	Adherence to approved protocol
Safety reporting	Adverse event documentation and reporting
Data recording	Accurate, complete, timely data entry

A1.3 Sponsor

Topic	Key Content
Quality management	System implementation, CtQ identification
Investigator selection	Qualification assessment
Protocol development	Scientific and ethical design
Safety evaluation	Ongoing benefit-risk assessment
Data management	Systems for reliable data collection
Monitoring	Risk-based monitoring strategy
Regulatory compliance	Submissions and communications

A1.4 Clinical Trial Protocol

Required Protocol Elements:

Category	Elements
General information	Title, sponsor ID, investigators, sites
Background	Scientific rationale, preclinical/clinical data
Objectives/Endpoints	Primary and secondary endpoints
Design	Study type, randomization, blinding
Population	Inclusion/exclusion criteria
Treatments	Dosing, administration, compliance
Assessments	Schedule of events, procedures
Safety	AE definitions, reporting requirements
Statistics	Sample size, analysis methods
Quality management	CtQ factors, risk mitigation

A1.5 Investigator's Brochure

Section	Content
Physical/Chemical	Drug substance properties
Nonclinical	Pharmacology, toxicology data
Clinical	PK, PD, safety, efficacy data
Guidance	Dosing, monitoring recommendations

A1.6 Essential Documents

Three Categories:

Before clinical phase begins: Regulatory approvals, protocol, IB, consent forms
During clinical conduct: CRFs, SAE reports, monitoring reports
After trial completion: Final reports, IP disposition, study report

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

Considerations for Remote Conduct:

Aspect	Guidance
Participant safety	Remote monitoring capabilities
Consent process	Electronic consent considerations
Data collection	Direct data capture methods
IP distribution	Direct-to-participant shipping
Oversight	Remote monitoring approaches

A2.2 Digital Health Technologies (DHTs)

Topic	Key Points
Validation	Fit-for-purpose validation requirements
Data integrity	Electronic systems controls
Participant training	Device usage instruction
Technical support	Help desk availability

A2.3 Non-Traditional Trial Designs

Addressed Designs:

Adaptive trials
Master protocols (basket, umbrella, platform)
Pragmatic trials
Real-world evidence integration

Key Changes from E6(R2)

Area	E6(R2)	E6(R3)
Structure	Single document	Principles + 2 Annexes
Principles	13 principles (Section 2)	11 overarching principles (Section II)
Quality management	Introduced RBQM	Central organizing principle
Technology	Limited guidance	Extensive DHT coverage
Flexibility	Prescriptive	Outcome-focused
Trial types	Traditional focus	Non-traditional addressed
Monitoring	Risk-based introduced	Centralized monitoring emphasized

Quick Reference: Section Finder

Looking for guidance on...

Topic	Primary Location
Informed consent	A1.2.5 (Investigator section)
Protocol amendments	A1.4.5
SAE reporting	A1.2.7 (Investigator), A1.3.8 (Sponsor)
Monitoring	A1.3.10
Essential documents	A1.6
Decentralized trials	A2.1
Electronic systems	A2.2
Source documentation	A1.2.8

Implementation Timeline

Region	Expected Implementation
ICH regions	Phased implementation through 2025-2026
FDA	Draft guidance aligned with E6(R3)
EMA	Incorporated into EU CTR framework

Verify current status with relevant regulatory authority as timelines evolve.

ICH E6(R3) Structure Overview

Document Architecture

Component	Purpose	Applicability
Overarching Principles	Foundational GCP principles	All clinical trials
Annex 1	Detailed requirements for interventional IMP trials	Interventional medicinal product trials
Annex 2	Additional considerations for non-traditional approaches	Decentralized trials, digital technologies, pragmatic trials

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Key Points:

Establishes scope applicable to interventional clinical trials of investigational medicinal products
Emphasizes human participant protection and data reliability
Introduces proportionate, risk-based approaches

Section 2: Principles of ICH E6(R3)

Principle	Title	Focus
Principle 1	Ethical Conduct and Participant Protection	Clinical trials should be conducted in accordance with ethical principles from the Declaration of Helsinki, consistent with GCP and applicable regulatory requirements. Rights, safety, and well-being of participants are paramount.
Principle 2	Informed Consent	Informed consent is integral to ethical trial conduct. Participation should be voluntary, based on a consent process ensuring participants are well-informed.
Principle 3	IRB/IEC Review	Clinical trials should be subject to independent review by an IRB/IEC with documented prior approval before trial initiation.
Principle 4	Scientific Soundness	Clinical trials should be scientifically sound for their intended purpose, based on adequate and current scientific knowledge and approaches.
Principle 5	Qualified Individuals	Clinical trials should be designed and conducted by individuals qualified by education, training, and experience.
Principle 6	Quality by Design	Quality should be built into the scientific and operational design and conduct of clinical trials, with focus on factors critical to quality.
Principle 7	Proportionate Risk-Based Approach	Trial processes, measures, and approaches should be proportionate to risks to participants and importance of data collected, avoiding unnecessary burden.
Principle 8	Protocol Requirements	Clinical trials should be described in a clear, concise, scientifically sound, and operationally feasible protocol.
Principle 9	Reliable Results	Clinical trials should generate reliable results with appropriate data systems, record management, and transparency through registration and results posting.
Principle 10	Roles and Responsibilities	Roles and responsibilities in clinical trials should be clear and documented appropriately, with sponsors and investigators retaining overall responsibility even when activities are delegated.
Principle 11	Investigational Product Management	Investigational products should be manufactured in accordance with applicable GMP standards and managed according to product specifications and trial protocol.

Key E6(R3) Enhancements:

Principles 6 and 7 introduce the risk-proportionate, quality-by-design approach central to E6(R3)
Principle 9 emphasizes data reliability, computerized systems validation, and trial transparency
Principle 10 addresses the complex ecosystem of sponsors, investigators, and service providers with clear accountability

Section 3: Quality Management

Critical Concepts:

Critical to Quality (CtQ) Factors: Elements essential to participant protection and data reliability
Risk-Based Quality Management: Prospective identification, assessment, and control of risks
Proportionality: Activities scaled to risk level of the trial

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

Topic	Key Content
Responsibilities	Protocol review, continuing review, safety monitoring
Composition	Qualified membership requirements
Documentation	Records of meetings, decisions, member qualifications

A1.2 Investigator

Topic	Key Content
Qualifications	Education, training, experience requirements
Resources	Adequate facilities, equipment, staff
Medical care	Participant medical decisions
Informed consent	Process and documentation
Protocol compliance	Adherence to approved protocol
Safety reporting	Adverse event documentation and reporting
Data recording	Accurate, complete, timely data entry

A1.3 Sponsor

Topic	Key Content
Quality management	System implementation, CtQ identification
Investigator selection	Qualification assessment
Protocol development	Scientific and ethical design
Safety evaluation	Ongoing benefit-risk assessment
Data management	Systems for reliable data collection
Monitoring	Risk-based monitoring strategy
Regulatory compliance	Submissions and communications

A1.4 Clinical Trial Protocol

Required Protocol Elements:

Category	Elements
General information	Title, sponsor ID, investigators, sites
Background	Scientific rationale, preclinical/clinical data
Objectives/Endpoints	Primary and secondary endpoints
Design	Study type, randomization, blinding
Population	Inclusion/exclusion criteria
Treatments	Dosing, administration, compliance
Assessments	Schedule of events, procedures
Safety	AE definitions, reporting requirements
Statistics	Sample size, analysis methods
Quality management	CtQ factors, risk mitigation

A1.5 Investigator's Brochure

Section	Content
Physical/Chemical	Drug substance properties
Nonclinical	Pharmacology, toxicology data
Clinical	PK, PD, safety, efficacy data
Guidance	Dosing, monitoring recommendations

A1.6 Essential Documents

Three Categories:

Before clinical phase begins: Regulatory approvals, protocol, IB, consent forms
During clinical conduct: CRFs, SAE reports, monitoring reports
After trial completion: Final reports, IP disposition, study report

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

Considerations for Remote Conduct:

Aspect	Guidance
Participant safety	Remote monitoring capabilities
Consent process	Electronic consent considerations
Data collection	Direct data capture methods
IP distribution	Direct-to-participant shipping
Oversight	Remote monitoring approaches

A2.2 Digital Health Technologies (DHTs)

Topic	Key Points
Validation	Fit-for-purpose validation requirements
Data integrity	Electronic systems controls
Participant training	Device usage instruction
Technical support	Help desk availability

A2.3 Non-Traditional Trial Designs

Addressed Designs:

Adaptive trials
Master protocols (basket, umbrella, platform)
Pragmatic trials
Real-world evidence integration

Key Changes from E6(R2)

Area	E6(R2)	E6(R3)
Structure	Single document	Principles + 2 Annexes
Principles	13 principles (Section 2)	11 overarching principles (Section II)
Quality management	Introduced RBQM	Central organizing principle
Technology	Limited guidance	Extensive DHT coverage
Flexibility	Prescriptive	Outcome-focused
Trial types	Traditional focus	Non-traditional addressed
Monitoring	Risk-based introduced	Centralized monitoring emphasized

Quick Reference: Section Finder

Looking for guidance on...

Topic	Primary Location
Informed consent	A1.2.5 (Investigator section)
Protocol amendments	A1.4.5
SAE reporting	A1.2.7 (Investigator), A1.3.8 (Sponsor)
Monitoring	A1.3.10
Essential documents	A1.6
Decentralized trials	A2.1
Electronic systems	A2.2
Source documentation	A1.2.8

Implementation Timeline

Region	Expected Implementation
ICH regions	Phased implementation through 2025-2026
FDA	Draft guidance aligned with E6(R3)
EMA	Incorporated into EU CTR framework

Verify current status with relevant regulatory authority as timelines evolve.

ICH E6(R3) Structure Overview

Document Architecture

Component	Purpose	Applicability
Overarching Principles	Foundational GCP principles	All clinical trials
Annex 1	Detailed requirements for interventional IMP trials	Interventional medicinal product trials
Annex 2	Additional considerations for non-traditional approaches	Decentralized trials, digital technologies, pragmatic trials

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Key Points:

Establishes scope applicable to interventional clinical trials of investigational medicinal products
Emphasizes human participant protection and data reliability
Introduces proportionate, risk-based approaches

Section 2: Principles of ICH E6(R3)

Principle	Title	Focus
Principle 1	Ethical Conduct and Participant Protection	Clinical trials should be conducted in accordance with ethical principles from the Declaration of Helsinki, consistent with GCP and applicable regulatory requirements. Rights, safety, and well-being of participants are paramount.
Principle 2	Informed Consent	Informed consent is integral to ethical trial conduct. Participation should be voluntary, based on a consent process ensuring participants are well-informed.
Principle 3	IRB/IEC Review	Clinical trials should be subject to independent review by an IRB/IEC with documented prior approval before trial initiation.
Principle 4	Scientific Soundness	Clinical trials should be scientifically sound for their intended purpose, based on adequate and current scientific knowledge and approaches.
Principle 5	Qualified Individuals	Clinical trials should be designed and conducted by individuals qualified by education, training, and experience.
Principle 6	Quality by Design	Quality should be built into the scientific and operational design and conduct of clinical trials, with focus on factors critical to quality.
Principle 7	Proportionate Risk-Based Approach	Trial processes, measures, and approaches should be proportionate to risks to participants and importance of data collected, avoiding unnecessary burden.
Principle 8	Protocol Requirements	Clinical trials should be described in a clear, concise, scientifically sound, and operationally feasible protocol.
Principle 9	Reliable Results	Clinical trials should generate reliable results with appropriate data systems, record management, and transparency through registration and results posting.
Principle 10	Roles and Responsibilities	Roles and responsibilities in clinical trials should be clear and documented appropriately, with sponsors and investigators retaining overall responsibility even when activities are delegated.
Principle 11	Investigational Product Management	Investigational products should be manufactured in accordance with applicable GMP standards and managed according to product specifications and trial protocol.

Key E6(R3) Enhancements:

Principles 6 and 7 introduce the risk-proportionate, quality-by-design approach central to E6(R3)
Principle 9 emphasizes data reliability, computerized systems validation, and trial transparency
Principle 10 addresses the complex ecosystem of sponsors, investigators, and service providers with clear accountability

Section 3: Quality Management

Critical Concepts:

Critical to Quality (CtQ) Factors: Elements essential to participant protection and data reliability
Risk-Based Quality Management: Prospective identification, assessment, and control of risks
Proportionality: Activities scaled to risk level of the trial

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

Topic	Key Content
Responsibilities	Protocol review, continuing review, safety monitoring
Composition	Qualified membership requirements
Documentation	Records of meetings, decisions, member qualifications

A1.2 Investigator

Topic	Key Content
Qualifications	Education, training, experience requirements
Resources	Adequate facilities, equipment, staff
Medical care	Participant medical decisions
Informed consent	Process and documentation
Protocol compliance	Adherence to approved protocol
Safety reporting	Adverse event documentation and reporting
Data recording	Accurate, complete, timely data entry

A1.3 Sponsor

Topic	Key Content
Quality management	System implementation, CtQ identification
Investigator selection	Qualification assessment
Protocol development	Scientific and ethical design
Safety evaluation	Ongoing benefit-risk assessment
Data management	Systems for reliable data collection
Monitoring	Risk-based monitoring strategy
Regulatory compliance	Submissions and communications

A1.4 Clinical Trial Protocol

Required Protocol Elements:

Category	Elements
General information	Title, sponsor ID, investigators, sites
Background	Scientific rationale, preclinical/clinical data
Objectives/Endpoints	Primary and secondary endpoints
Design	Study type, randomization, blinding
Population	Inclusion/exclusion criteria
Treatments	Dosing, administration, compliance
Assessments	Schedule of events, procedures
Safety	AE definitions, reporting requirements
Statistics	Sample size, analysis methods
Quality management	CtQ factors, risk mitigation

A1.5 Investigator's Brochure

Section	Content
Physical/Chemical	Drug substance properties
Nonclinical	Pharmacology, toxicology data
Clinical	PK, PD, safety, efficacy data
Guidance	Dosing, monitoring recommendations

A1.6 Essential Documents

Three Categories:

Before clinical phase begins: Regulatory approvals, protocol, IB, consent forms
During clinical conduct: CRFs, SAE reports, monitoring reports
After trial completion: Final reports, IP disposition, study report

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

Considerations for Remote Conduct:

Aspect	Guidance
Participant safety	Remote monitoring capabilities
Consent process	Electronic consent considerations
Data collection	Direct data capture methods
IP distribution	Direct-to-participant shipping
Oversight	Remote monitoring approaches

A2.2 Digital Health Technologies (DHTs)

Topic	Key Points
Validation	Fit-for-purpose validation requirements
Data integrity	Electronic systems controls
Participant training	Device usage instruction
Technical support	Help desk availability

A2.3 Non-Traditional Trial Designs

Addressed Designs:

Adaptive trials
Master protocols (basket, umbrella, platform)
Pragmatic trials
Real-world evidence integration

Key Changes from E6(R2)

Area	E6(R2)	E6(R3)
Structure	Single document	Principles + 2 Annexes
Principles	13 principles (Section 2)	11 overarching principles (Section II)
Quality management	Introduced RBQM	Central organizing principle
Technology	Limited guidance	Extensive DHT coverage
Flexibility	Prescriptive	Outcome-focused
Trial types	Traditional focus	Non-traditional addressed
Monitoring	Risk-based introduced	Centralized monitoring emphasized

Quick Reference: Section Finder

Looking for guidance on...

Topic	Primary Location
Informed consent	A1.2.5 (Investigator section)
Protocol amendments	A1.4.5
SAE reporting	A1.2.7 (Investigator), A1.3.8 (Sponsor)
Monitoring	A1.3.10
Essential documents	A1.6
Decentralized trials	A2.1
Electronic systems	A2.2
Source documentation	A1.2.8

Implementation Timeline

Region	Expected Implementation
ICH regions	Phased implementation through 2025-2026
FDA	Draft guidance aligned with E6(R3)
EMA	Incorporated into EU CTR framework

Verify current status with relevant regulatory authority as timelines evolve.

ICH E6(R3) Key Sections At-a-Glance

ICH E6(R3) Structure Overview

Document Architecture

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Section 2: Principles of ICH E6(R3)

Section 3: Quality Management

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

A1.2 Investigator

A1.3 Sponsor

A1.4 Clinical Trial Protocol

A1.5 Investigator's Brochure

A1.6 Essential Documents

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

A2.2 Digital Health Technologies (DHTs)

A2.3 Non-Traditional Trial Designs

Key Changes from E6(R2)

Quick Reference: Section Finder

Implementation Timeline

Was this resource helpful?

Author

Dr. Sarah Chen

Tags

Related Resources

SAE Reporting Timeline Quick Reference

Clinical Trial Roles Quick Reference

Protocol Deviation Classification Quick Reference

ICH E6(R3) Key Sections At-a-Glance

ICH E6(R3) Structure Overview

Document Architecture

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Section 2: Principles of ICH E6(R3)

Section 3: Quality Management

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

A1.2 Investigator

A1.3 Sponsor

A1.4 Clinical Trial Protocol

A1.5 Investigator's Brochure

A1.6 Essential Documents

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

A2.2 Digital Health Technologies (DHTs)

A2.3 Non-Traditional Trial Designs

Key Changes from E6(R2)

Quick Reference: Section Finder

Implementation Timeline

Was this resource helpful?

Author

Dr. Sarah Chen

Tags

Related Resources

SAE Reporting Timeline Quick Reference

Clinical Trial Roles Quick Reference

Protocol Deviation Classification Quick Reference

ICH E6(R3) Key Sections At-a-Glance

ICH E6(R3) Structure Overview

Document Architecture

Overarching Principles (Sections 1-3)

Section 1: Introduction and Purpose

Section 2: Principles of ICH E6(R3)

Section 3: Quality Management

Annex 1: Interventional Clinical Trials of Investigational Medicinal Products

A1.1 Institutional Review Board/Independent Ethics Committee

A1.2 Investigator

A1.3 Sponsor

A1.4 Clinical Trial Protocol

A1.5 Investigator's Brochure

A1.6 Essential Documents

Annex 2: Additional Considerations

A2.1 Decentralized Clinical Trials (DCTs)

A2.2 Digital Health Technologies (DHTs)

A2.3 Non-Traditional Trial Designs

Key Changes from E6(R2)

Quick Reference: Section Finder

Implementation Timeline

Was this resource helpful?