Analytical Method Development: Isocratic Method Optimization SOP – V 2.0

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Analytical Method Development: Isocratic Method Optimization SOP – V 2.0

SOP for Optimization of Isocratic HPLC Methods in Analytical Method Development


Department Analytical Method Development
SOP No. SOP/AMD/070/2025
Supersedes SOP/AMD/070/2022
Page No. Page 1 of 14
Issue Date 19/05/2025
Effective Date 20/05/2025
Review Date 19/05/2026

1. Purpose

This SOP outlines a structured approach for the optimization of isocratic HPLC methods used for analyzing pharmaceutical substances. It includes the selection of suitable columns, mobile phase composition, buffer strength,

detection wavelength, and flow rate to achieve reproducible retention times and efficient separation with minimal baseline noise.

2. Scope

This SOP applies to all activities within the Analytical Method Development (AMD) laboratory related to optimizing isocratic HPLC methods for raw materials, APIs, excipients, and finished pharmaceutical products when gradient methods are not required or preferred.

3. Responsibilities

  • Analytical Chemist: Executes method trials, records data, interprets chromatograms, and suggests optimization changes.
  • Reviewer: Reviews method optimization sheets and approves final isocratic method conditions.
  • QA Officer: Ensures regulatory compliance and documentation completeness.
  • Head – AMD: Approves the optimized method and authorizes its use in method validation or transfer.
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4. Accountability

The Head of AMD is accountable for ensuring the optimized isocratic methods meet analytical performance and regulatory standards.

5. Procedure

5.1 Initial Method Setup

  1. Begin with default isocratic conditions using 60:40 (v/v) water:acetonitrile or water:methanol as mobile phase.
  2. Select a reversed-phase C18 column (150 mm × 4.6 mm, 5 µm particle size) for general testing unless the API is hydrophilic or ionic.
  3. Choose detection wavelength based on UV absorbance maxima from PDA scan or literature.
  4. Set flow rate to 1.0 mL/min and column temperature at 30°C initially.
  5. Document initial method parameters in Annexure-1: Method Initialization Log.

5.2 Retention Time and Peak Shape Evaluation

  1. Inject standard API solution and observe:
    • Retention time (target 2–10 min)
    • Peak shape and tailing factor (≤ 2.0)
    • Theoretical plates (≥ 2000)
  2. If API elutes too early (<1.5 min), increase aqueous content; if too late (>12 min), increase organic content.
  3. Adjust flow rate if needed for retention tuning.
  4. Document observations in Annexure-2: Retention Optimization Log.

5.3 Mobile Phase Selection and Adjustment

  1. Select the optimal organic solvent (ACN vs MeOH) based on peak sharpness and resolution.
  2. Use buffer in aqueous phase if the API is ionizable:
    • Buffer range: pH 3.0–7.0 (e.g., phosphate, acetate)
    • Buffer strength: 10–20 mM
  3. Maintain buffer solubility and compatibility with UV detection.
  4. Record buffer details and mobile phase adjustments in Annexure-3: Mobile Phase Optimization Sheet.

5.4 Method Robustness Trials

  1. Assess the effect of small deliberate variations:
    • ±0.2 mL/min flow rate
    • ±2°C column oven temperature
    • ±2% change in mobile phase ratio
  2. Evaluate peak area, resolution, and retention time drift.
  3. Document results in Annexure-4: Robustness Evaluation Log.

5.5 Final Method Parameters

  1. Summarize optimized parameters:
    • Mobile phase ratio (A:B)
    • pH and buffer strength
    • Flow rate
    • Injection volume
    • Run time
  2. Confirm system suitability with 5 replicate injections.
  3. Transfer method to validation phase after approval.
  4. Enter finalized conditions in Annexure-5: Final Optimized Method Record.

6. Abbreviations

  • HPLC: High Performance Liquid Chromatography
  • API: Active Pharmaceutical Ingredient
  • UV: Ultraviolet
  • PDA: Photodiode Array
  • SOP: Standard Operating Procedure

7. Documents

  1. Method Initialization Log – Annexure-1
  2. Retention Optimization Log – Annexure-2
  3. Mobile Phase Optimization Sheet – Annexure-3
  4. Robustness Evaluation Log – Annexure-4
  5. Final Optimized Method Record – Annexure-5

8. References

  • USP General Chapter <621> – Chromatography
  • ICH Q2(R1) – Validation of Analytical Procedures
  • FDA Guidance on Analytical Procedures and Methods Validation

9. SOP Version

Version: 2.0

10. Approval Section

Prepared By Checked By Approved By
Signature
Date
Name
Designation
Department

11. Annexures

Annexure-1: Method Initialization Log

Column Mobile Phase Flow Rate Detection Temperature
C18, 150 × 4.6 mm Water:ACN (60:40) 1.0 mL/min UV 254 nm 30°C

Annexure-2: Retention Optimization Log

Trial Retention Time Tailing Resolution Remarks
1 2.3 1.2 N/A Too early elution

Annexure-3: Mobile Phase Optimization Sheet

Trial A:B Ratio pH Peak Shape Conclusion
2 70:30 4.5 Sharp Accepted

Annexure-4: Robustness Evaluation Log

Parameter Variation Impact Status
Flow Rate 0.8 mL/min Slight increase in retention time Acceptable

Annexure-5: Final Optimized Method Record

Column Mobile Phase Flow Rate Detection Injection Volume Run Time
C18 70:30 Water:ACN 1.0 mL/min 254 nm 20 µL 10 min

Revision History:

Revision Date Revision No. Details Reason Approved By
04/05/2025 2.0 Expanded optimization trials, added robustness testing Annual SOP Review
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