Standard Operating Procedure for Dilution Integrity Testing in BA/BE Bioanalytical Validation

Department	BA-BE Studies
SOP No.	SOP/BA-BE/181/2025
Supersedes	SOP/BA-BE/181/2022
Page No.	Page 1 of 8
Issue Date	17/04/2025
Effective Date	20/04/2025
Review Date	17/04/2026

1. Purpose

To define the procedure for evaluating dilution integrity during method validation of LC-MS/MS methods for bioavailability/bioequivalence (BA/BE) studies, ensuring accurate quantification of samples above the upper limit of quantification (ULOQ) after dilution.

2. Scope

This SOP applies to all validated bioanalytical methods in BA/BE studies involving plasma sample analysis where dilution is required for samples exceeding the calibration range.

3. Responsibilities

• Analyst: Prepares dilution integrity samples and performs analysis according to protocol.
• Supervisor: Reviews dilution data, verifies calculations, and confirms result validity.
• QA Officer: Ensures that documentation, acceptance criteria, and reporting comply with ICH M10 and FDA requirements.

4. Accountability

The Bioanalytical Laboratory Head is accountable for ensuring that dilution integrity tests are executed, evaluated, and reported as part of the method validation dossier.

5. Procedure

5.1 Sample Preparation

1. Prepare a stock solution at a concentration above the ULOQ (typically 1.5–2 times ULOQ).
2. Prepare at least five replicates of diluted samples using blank plasma to achieve target dilution levels (e.g., 1:5, 1:10).
3. Label each sample appropriately, including dilution factor, QC level, and preparation date.
4. Document all preparation steps in Annexure-1: Dilution Integrity Preparation Log.

5.2 Analysis

1. Analyze diluted samples with a freshly prepared calibration curve covering the validated range.
2. Inject diluted samples using validated LC-MS/MS method and record analyte response.
3. Calculate the concentration using the dilution factor applied to back-calculated values.

5.3 Acceptance Criteria

1. Accuracy should be within ±15% of the nominal concentration after applying dilution.
2. Precision (%CV) must be ≤15% across replicates.
3. Any deviations or failures must be documented with rationale and justification.
4. Record results in Annexure-2: Dilution Integrity Result Summary.

5.4 Documentation and Reporting

1. Attach chromatograms, calculations, and accuracy/precision reports for each dilution set.
2. Prepare a summary and include in the method validation report.
3. Submit documentation to QA for approval and archival.

6. Abbreviations

• BA/BE: Bioavailability/Bioequivalence
• ULOQ: Upper Limit of Quantification
• %CV: Percent Coefficient of Variation
• QA: Quality Assurance

7. Documents

1. Dilution Integrity Preparation Log – Annexure-1
2. Dilution Integrity Result Summary – Annexure-2

8. References

• ICH M10: Bioanalytical Method Validation
• US FDA Guidance for Industry: Bioanalytical Method Validation (2022)
• Internal Method Validation Protocol

9. SOP Version

Version: 2.0

10. Approval Section

	Prepared By	Checked By	Approved By
Signature
Date
Name
Designation
Department

11. Annexures

Annexure-1: Dilution Integrity Preparation Log

Sample ID	Nominal Conc. (ng/mL)	Dilution Factor	Prepared Conc.	Prepared By	Date
DI-01	4000	1:5	800	Rajesh Kumar	16/04/2025

Annexure-2: Dilution Integrity Result Summary

Replicate	Back Calculated Conc. (ng/mL)	Nominal Conc.	% Accuracy	Status
1	810	800	101.2%	Accepted
2	788	800	98.5%	Accepted

Revision History:

Revision Date	Revision No.	Details	Reason	Approved By
01/01/2022	1.0	Initial SOP Release	New SOP	QA Head
17/04/2025	2.0	Revised procedure with expanded documentation templates	ICH M10 Compliance	QA Head