clinical trial documentation retention – Clinical Research Made Simple https://www.clinicalstudies.in Trusted Resource for Clinical Trials, Protocols & Progress Sun, 21 Sep 2025 15:25:50 +0000 en-US hourly 1 https://wordpress.org/?v=6.9.1 SOP for Record Retention (Global Durations and Triggers) https://www.clinicalstudies.in/sop-for-record-retention-global-durations-and-triggers/ Sun, 21 Sep 2025 15:25:50 +0000 ]]> https://www.clinicalstudies.in/?p=7031 Read More “SOP for Record Retention (Global Durations and Triggers)” »

]]> SOP for Record Retention (Global Durations and Triggers)

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Standard Operating Procedure for Record Retention (Global Durations and Triggers)

SOP No. CR/OPS/090/2025
Supersedes NA
Page No. 1 of 44
Issue Date 26/08/2025
Effective Date 01/09/2025
Review Date 01/09/2026

Purpose

The purpose of this SOP is to establish standardized procedures for record retention in clinical trials, defining global durations and triggers that align with ICH GCP, FDA, EMA, CDSCO, WHO, GDPR, and HIPAA requirements. Proper record retention ensures availability of essential documents for audits, inspections, pharmacovigilance, and legal defense.

Scope

This SOP applies to sponsors, investigators, CROs, QA, and vendors involved in maintaining clinical trial documentation. It covers retention and archiving of Trial Master File (TMF), Investigator Site File (ISF), laboratory data, pharmacovigilance records, informed consent forms, electronic data, and subject safety information.

Responsibilities

  • Sponsor: Defines record retention policy and ensures global compliance.
  • Investigator: Maintains ISF and site-level essential records.
  • QA: Audits record retention practices and verifies compliance.
  • Data Management: Maintains electronic records and databases.
  • Vendors: Archive and retain outsourced records securely.

Accountability

The Sponsor is accountable for defining retention timelines and ensuring implementation across regions. QA is accountable for oversight of retention records and inspection readiness.

Procedure

1. Retention Durations by Region
1.1 FDA (US): Retain essential records for at least 2 years after the last marketing approval or trial discontinuation.
1.2 EMA (EU): Retain essential documents for 25 years or longer if required by protocol.
1.3 CDSCO (India): Retain trial records for minimum 5 years after completion.
1.4 WHO: Recommend retention of critical records for 15 years.
1.5 GDPR/HIPAA: Retention must also respect privacy laws and subject rights.

2. Retention Triggers
2.1 Records must be retained until the last marketing approval or withdrawal of product.
2.2 Pharmacovigilance records must be retained as per DSUR/PSUR requirements.
2.3 Retain subject safety and informed consent forms per protocol and regional laws.

3. Types of Records
3.1 TMF and ISF essential documents.
3.2 Source documents and CRFs.
3.3 Safety and pharmacovigilance reports (SAE, SUSAR, DSUR, PSUR).
3.4 Laboratory raw data, calibration logs, and validation reports.
3.5 Training, monitoring, and audit reports.

4. Storage Requirements
4.1 Store paper records in secure, access-controlled facilities.
4.2 Archive electronic records in validated eSystems with audit trails.
4.3 Perform periodic data integrity checks.

5. Destruction
5.1 Destruction is permitted only after retention timelines expire and with sponsor approval.
5.2 Maintain Certificate of Destruction (Annexure-1).

6. Inspection Readiness
6.1 All retained records must be easily retrievable for regulatory inspections.
6.2 Maintain Record Retention Log (Annexure-2).

Abbreviations

  • SOP: Standard Operating Procedure
  • TMF: Trial Master File
  • ISF: Investigator Site File
  • FDA: Food and Drug Administration
  • EMA: European Medicines Agency
  • CDSCO: Central Drugs Standard Control Organization
  • WHO: World Health Organization
  • DSUR: Development Safety Update Report
  • PSUR: Periodic Safety Update Report
  • CRF: Case Report Form
  • QA: Quality Assurance

Documents

  1. Certificate of Destruction (Annexure-1)
  2. Record Retention Log (Annexure-2)

References

Version: 1.0

Approval Section

Prepared By Ravi Kumar, Clinical Archivist
Checked By Sunita Reddy, QA Officer
Approved By Dr. Anil Sharma, Head Clinical Quality

Annexures

Annexure-1: Certificate of Destruction

Date Record Type Method Witness Vendor
15/09/2035 Old ISF Records Shredding QA Officer ABC Archival Pvt Ltd

Annexure-2: Record Retention Log

Date Record Type Retention Duration Location Responsible
01/09/2025 TMF Documents 25 years Central Archive – Pune Archivist
01/09/2025 ISF Records 15 years Site Archive Site Coordinator

Revision History

Revision Date Revision No. Revision Details Reason for Revision Approved By
26/08/2025 00 Initial version New SOP creation Head Clinical Quality

For more SOPs visit: Pharma SOP

]]> Retention Requirements for Deviation Documentation https://www.clinicalstudies.in/retention-requirements-for-deviation-documentation/ Mon, 08 Sep 2025 07:04:29 +0000 https://www.clinicalstudies.in/?p=6605 Read More “Retention Requirements for Deviation Documentation” »

]]> Retention Requirements for Deviation Documentation

Retention Guidelines for Deviation Documentation in Clinical Research

Why Deviation Documentation Must Be Retained

Protocol deviations are critical records in clinical trials, providing evidence of trial conduct, subject protection, and regulatory compliance. Retaining deviation documentation is not optional—it is a core expectation under ICH-GCP, FDA, EMA, and other regional guidelines. These records help stakeholders assess trial integrity during audits, inspections, and regulatory submissions. Additionally, deviation documentation supports ongoing quality assurance, RCA reviews, and CAPA effectiveness assessments.

Improper or inconsistent retention of deviation logs and associated records may result in inspection findings, data exclusion, or even marketing application delays. This article outlines regulatory requirements and best practices for deviation documentation retention across the clinical trial lifecycle.

ICH-GCP and Regulatory Expectations for Retention

As per ICH E6(R2) Section 4.9.5 and 8.3, the following expectations apply:

  • Essential documents should be retained for at least 2 years after the last approval of a marketing application in an ICH region (or until there are no pending applications).
  • If the trial is discontinued prematurely, documents must be retained for at least 2 years after the discontinuation date.
  • Sponsors and investigators must agree in writing on who retains the trial documents and for how long.

Deviation records fall under essential documents because they contribute to understanding trial conduct and potential impact on data integrity. These records must be readily accessible and organized for inspection at any time.

Types of Deviation Documentation That Require Retention

The following types of records related to deviations must be retained:

  • Signed deviation reports by site staff or investigators
  • Deviation logs and tracking spreadsheets
  • CAPA plans associated with deviations
  • Root Cause Analysis (RCA) forms
  • Correspondence with sponsors or CROs regarding deviations
  • Meeting notes where deviation handling was discussed
  • Audit trail printouts (for electronic systems)
  • Deviation resolution status and closure documentation

These documents may exist in both electronic and paper formats. Consistency in the medium and clarity in documentation versioning is essential for compliance.

Electronic Systems and 21 CFR Part 11 Compliance

When using electronic deviation logging systems, sponsors and CROs must ensure:

  • System validation is complete and documented.
  • Audit trails are enabled and retained along with the deviation record.
  • Version control is active to capture edits, updates, and closures.
  • Electronic records are backed up regularly and securely stored.
  • User access logs are retained as part of deviation tracking metadata.

For U.S.-based trials, these systems must comply with 21 CFR Part 11 for electronic records and signatures. Systems should be validated to demonstrate data integrity and ensure ALCOA+ compliance (Attributable, Legible, Contemporaneous, Original, Accurate, plus Complete, Consistent, Enduring, and Available).

Retention Duration Based on Region

Region Minimum Retention Period Guidance/Authority
United States 2 years after final marketing approval FDA 21 CFR 312.62(c)
European Union 25 years (per EU CTR 536/2014) EMA
India 5 years or per DCGI requirement CDSCO
Japan 15 years PMDA

Note: The stricter retention policy (sponsor vs. investigator site) typically prevails unless otherwise agreed in a contractual document.

Deviation Documentation in the Trial Master File (TMF)

Deviation documents must be filed in the Trial Master File (TMF) under the appropriate section. For example:

  • Section 05.04.05: Protocol deviation documentation
  • Section 08.02.06: Monitoring visit reports citing deviations
  • Section 08.03.05: Communication related to deviations and CAPAs

Proper indexing and filing in TMF ensure easy retrieval during audits and inspections. Sponsors using eTMF systems like Veeva or PhlexTMF must verify metadata fields include deviation status, site number, and closure status.

Backup, Disaster Recovery, and Site Closeout Considerations

During site closeout and database lock, deviation records must be reconciled and archived:

  • All deviations must be closed, with documentation uploaded to TMF.
  • Signed deviation logs and any handwritten notes must be scanned and uploaded.
  • Disaster recovery plans should include deviation logs and ensure redundancy.
  • Site staff must confirm no paper deviation records remain unarchived.

Retention responsibility may shift to the sponsor or CRO post-site closeout depending on contract terms. Site master file checklists should include deviation documentation status.

Global Registry Disclosures and Deviation Transparency

While not mandatory for all registries, some public trial databases may require brief descriptions of major deviations disclosed in final results. Sponsors are encouraged to review registry-specific requirements such as:

Deviation documentation should be used to prepare accurate and transparent disclosures without compromising subject confidentiality.

Conclusion: Retention as a Cornerstone of Inspection Readiness

Retention of deviation documentation is not just a compliance requirement—it is a quality assurance safeguard that supports subject safety, regulatory transparency, and sponsor credibility. Sponsors and sites must establish SOPs, contract agreements, and e-system validations that ensure all deviation-related records are retained securely, completely, and accessibly for the required duration.

Proper retention practices not only withstand inspections—they demonstrate a commitment to ethical and compliant trial conduct.

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