conditions

Volume and number of aliquots

Pre-labeled or site-labeled tubes (with specifications)

Temperature and handling conditions

Documentation and labeling procedures

Deviation management and contingency procedures

Regulatory Expectations and ICH Guidelines

Regulatory authorities expect sponsors and CROs to define, implement, and monitor SOPs that ensure the quality and traceability of clinical samples. Key guidance includes:

• FDA: Requires adherence to CFR 21 Part 58 (GLP) and Part 312 for clinical trials, including accurate recording of sample origin, condition, and chain of custody.
• EMA: Refers to EudraLex Volume 10 and notes that sample handling is a key GCP compliance area during inspections.
• ICH-GCP: E6(R2) and E8(R1) recommend risk-based oversight and protocol-defined procedures for all biospecimen handling steps.

Table: Sample Collection SOP Checklist

Item	Description	Required?
Tube Type & Labeling	EDTA, SST, or heparin tubes with barcodes	Yes
Collection Volume	5–10 mL per timepoint per subject	Yes
Documentation Log	Sample collection CRF with timestamps	Yes
Cold Chain Procedure	2–8°C with gel packs; dry ice for frozen	Yes
Deviation Handling	Procedure for hemolysis, labeling errors	Yes

Case Study: FDA 483 Observation Due to Poor Sample Labeling

In a Phase III oncology trial, an FDA inspection noted inconsistent labeling of blood samples collected across different sites. Some tubes lacked subject IDs, while others were labeled in permanent marker without barcodes. This led to a 483 observation and a demand for immediate CAPA.

CAPA Steps Implemented:

• Developed a barcode-based labeling SOP with site training
• Conducted refresher training across all sites
• Implemented pre-labeled kits for time-sensitive visits
• Added a sample reconciliation step to the monitoring visit checklist

The CAPA was closed within 30 days and accepted by the FDA without the need for re-inspection.

Chain of Custody and Audit Trails

Sample custody should be traceable from collection to analysis. Each step—collection, labeling, interim storage, packaging, and shipment—should be time-logged with personnel initials. Use of electronic sample tracking software, such as FreezerPro, LabVantage, or ELPRO, is encouraged.

Logs should be stored in the Trial Master File (TMF) and/or electronic data capture (EDC) system. Deviations such as missed samples, incorrect timepoints, or packaging non-compliance should be logged with rationale.

Training Site Personnel and GCP Compliance

All staff involved in sample collection must receive role-specific training, including:

• Phlebotomy technique (if applicable)
• Labeling and documentation procedures
• Cold chain management
• Packaging for IATA-compliant shipping

Training logs should be maintained and reviewed prior to audits or inspections.

External Reference Example

For more detailed global practices, refer to ongoing sample-based research on Canada’s Clinical Trials Database, which includes studies emphasizing biospecimen integrity across phases.

Conclusion

Consistency and compliance in sample collection are fundamental to trial success. Implementing robust SOPs, training site staff, and employing a feedback-driven CAPA system ensures sample integrity and regulatory approval. With increasing focus from regulators on biospecimen traceability, sponsors must proactively audit and enhance their sample collection practices across all global sites.