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Guideline for good clinical practice E6(R2)

1 December 2016. EMA/CHMP/ICH/135/1995. Committee for Human Medicinal Products Guideline for good clinical practice E6(R2). Step 5. Adopted by CHMP for release for consultation 23 July 2015. Start of public consultation 4 August 2015. End of consultation (deadline for comments) 3 February 2016. Final adoption by CHMP 15 December 2016. Date for coming into effect 14 June 2017. 30 Churchill Place Canary Wharf London E14 5EU United Kingdom Telephone +44 (0)20 3660 6000 Facsimile +44 (0)20 3660 5555. Send a question via our website An agency of the European Union European Medicines Agency, 2017. Reproduction is authorised provided the source is acknowledged. Document History New First Codification History Date Codification November 2005. E6 Approval by the CPMP under Step 3 and release for May 1995 E6. public consultation. E6 Approval by the CPMP under Step 4 and released for July 1996 E6.

Guideline for good clinical practice E6(R2) EMA/CHMP/ICH/135/1995 Page 5/70 Introduction Good Clinical Practice (GCP) is an international ethical and scientific quality standard for

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Transcription of Guideline for good clinical practice E6(R2)

1 1 December 2016. EMA/CHMP/ICH/135/1995. Committee for Human Medicinal Products Guideline for good clinical practice E6(R2). Step 5. Adopted by CHMP for release for consultation 23 July 2015. Start of public consultation 4 August 2015. End of consultation (deadline for comments) 3 February 2016. Final adoption by CHMP 15 December 2016. Date for coming into effect 14 June 2017. 30 Churchill Place Canary Wharf London E14 5EU United Kingdom Telephone +44 (0)20 3660 6000 Facsimile +44 (0)20 3660 5555. Send a question via our website An agency of the European Union European Medicines Agency, 2017. Reproduction is authorised provided the source is acknowledged. Document History New First Codification History Date Codification November 2005. E6 Approval by the CPMP under Step 3 and release for May 1995 E6. public consultation. E6 Approval by the CPMP under Step 4 and released for July 1996 E6.

2 Information. Step 5 corrected version E6 Approval by the CPMP of Post-Step 4 editorial July 2002 E6(R1). corrections. Current E6(R2) Addendum Step 5 version Code History Date E6 Approval by the Steering Committee under Step 2 and release for 11 June public consultation. 2015. Integrated Addendum to ICH E6(R1) document. Changes are integrated directly into the following sections of the parental Guideline : Introduction, , , , , , , , , , , , , , , , , , , , , , , , Guideline for good clinical practice E6(R2). EMA/CHMP/ICH/135/1995 Page 2/70. Guideline for good clinical practice E6(R2). Table of contents Introduction .. 5. 1. Glossary .. 6. 2. The principles of ICH GCP .. 14. 3. Institutional Review Board / Independent Ethics Committee (IRB/IEC).. 15. Responsibilities .. 15. Composition, Functions and Operations .. 17. Procedures .. 17. Records.

3 19. 4. Investigator .. 19. Investigator's Qualifications and Agreements .. 19. Adequate Resources .. 19. Medical Care of Trial Subjects .. 20. Communication with IRB/IEC .. 21. Compliance with Protocol .. 21. Investigational Product(s) .. 22. Randomization Procedures and Unblinding .. 23. Informed Consent of Trial Subjects .. 23. Records and Reports .. 26. Progress Reports .. 28. Safety Reporting .. 28. Premature Termination or Suspension of a 28. Final Report(s) by Investigator .. 29. 5. Sponsor .. 29. Quality management .. 29. Quality assurance and quality control .. 30. Contract Research Organization (CRO) .. 31. Medical expertise .. 31. Trial 32. Trial management, data handling, and record keeping .. 32. Investigator 34. Allocation of responsibilities .. 35. Compensation to subjects and investigators .. 35. Financing .. 35. Notification/submission to regulatory authority(ies).

4 35. Confirmation of review by IRB/IEC .. 35. The sponsor should obtain from the investigator/institution: .. 35. Information on investigational product(s) .. 36. Manufacturing, packaging, labelling, and coding investigational product(s) .. 36. Guideline for good clinical practice E6(R2). EMA/CHMP/ICH/135/1995 Page 3/70. Supplying and handling investigational product(s) .. 37. Record access .. 38. Safety information .. 38. Adverse drug reaction reporting .. 38. Monitoring .. 39. Audit .. 42. Noncompliance .. 43. Premature termination or suspension of a trial .. 43. clinical trial/study reports .. 44. Multicentre trials .. 44. 6. clinical trial protocol and protocol amendment(s).. 45. General Information .. 45. Background Information .. 45. Trial objectives and purpose .. 46. Trial 46. Selection and withdrawal of 47. Treatment of 48. Assessment of Efficacy.

5 48. Assessment of 48. Statistics .. 49. Direct access to source data/documents .. 49. Quality control and quality assurance .. 49. Ethics .. 49. Data handling and record 50. Financing and insurance .. 50. Publication policy .. 50. Supplements .. 50. 7. Investigator's brochure .. 51. 51. General considerations .. 51. Contents of the investigator's brochure .. 52. Appendix 1: .. 56. Appendix 2: .. 57. 8. Essential documents for the conduct of a clinical trial .. 58. 58. Before the clinical phase of the trial commences .. 59. During the clinical Conduct of the Trial .. 63. After Completion or Termination of the Trial .. 69. Guideline for good clinical practice E6(R2). EMA/CHMP/ICH/135/1995 Page 4/70. Introduction good clinical practice (GCP) is an international ethical and scientific quality standard for designing, conducting, recording and reporting trials that involve the participation of human subjects.

6 Compliance with this standard provides public assurance that the rights, safety and well-being of trial subjects are protected, consistent with the principles that have their origin in the Declaration of Helsinki, and that the clinical trial data are credible. The objective of this ICH GCP Guideline is to provide a unified standard for the European Union (EU), Japan and the United States to facilitate the mutual acceptance of clinical data by the regulatory authorities in these jurisdictions. The Guideline was developed with consideration of the current good clinical practices of the European Union, Japan, and the United States, as well as those of Australia, Canada, the Nordic countries and the World Health Organization (WHO). This Guideline should be followed when generating clinical trial data that are intended to be submitted to regulatory authorities.

7 The principles established in this Guideline may also be applied to other clinical investigations that may have an impact on the safety and well-being of human subjects. ADDENDUM. Since the development of the ICH GCP Guideline , the scale, complexity, and cost of clinical trials have increased. Evolutions in technology and risk management processes offer new opportunities to increase efficiency and focus on relevant activities. When the original ICH E6(R1) text was prepared, clinical trials were performed in a largely paper-based process. Advances in use of electronic data recording and reporting facilitate implementation of other approaches. For example, centralized monitoring can now offer a greater advantage, to a broader range of trials than is suggested in the original text. Therefore, this Guideline has been amended to encourage implementation of improved and more efficient approaches to clinical trial design, conduct, oversight, recording and reporting while continuing to ensure human subject protection and reliability of trial results.

8 Standards regarding electronic records and essential documents intended to increase clinical trial quality and efficiency have also been updated. This Guideline should be read in conjunction with other ICH guidelines relevant to the conduct of clinical trials ( , E2A ( clinical safety data management), E3 ( clinical study reporting), E7 (geriatric populations), E8 (general considerations for clinical trials), E9 (statistical principles), and E11 (pediatric populations)). This ICH GCP Guideline Integrated Addendum provides a unified standard for the European Union, Japan, the United States, Canada, and Switzerland to facilitate the mutual acceptance of data from clinical trials by the regulatory authorities in these jurisdictions. In the event of any conflict between the E6(R1) text and the E6(R2) addendum text, the E6(R2) addendum text should take priority.

9 Guideline for good clinical practice E6(R2). EMA/CHMP/ICH/135/1995 Page 5/70. 1. Glossary Adverse Drug Reaction (ADR). In the pre-approval clinical experience with a new medicinal product or its new usages, particularly as the therapeutic dose(s) may not be established: all noxious and unintended responses to a medicinal product related to any dose should be considered adverse drug reactions. The phrase responses to a medicinal product means that a causal relationship between a medicinal product and an adverse event is at least a reasonable possibility, the relationship cannot be ruled out. Regarding marketed medicinal products: a response to a drug which is noxious and unintended and which occurs at doses normally used in man for prophylaxis, diagnosis, or therapy of diseases or for modification of physiological function (see the ICH Guideline for clinical Safety Data Management: Definitions and Standards for Expedited Reporting).

10 Adverse Event (AE). Any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have a causal relationship with this treatment. An adverse event (AE) can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding), symptom, or disease temporally associated with the use of a medicinal (investigational) product, whether or not related to the medicinal (investigational) product (see the ICH Guideline for clinical Safety Data Management: Definitions and Standards for Expedited Reporting). Amendment (to the protocol). See Protocol Amendment. Applicable regulatory requirement(s). Any law(s) and regulation(s) addressing the conduct of clinical trials of investigational products. Approval (in relation to institutional review boards).


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