SOP Guide for Pharma

Analytical Method Development: LC-MS Method Development – V 2.0

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Analytical Method Development: LC-MS Method Development – V 2.0

Standard Operating Procedure for LC-MS Method Development in Analytical Method Development


Department Analytical Method Development
SOP No. SOP/AMD/106/2025
Supersedes SOP/AMD/106/2022
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 provides a comprehensive procedure for the development of Liquid Chromatography–Mass Spectrometry (LC-MS) methods used for qualitative and quantitative determination of drug substances, degradation products, and impurities in pharmaceutical products.

2. Scope

This procedure applies to all LC-MS method development activities within the Analytical Method Development (AMD) laboratory involving small molecules and selected large molecules where mass-based detection is required.

3. Responsibilities

  • Analytical Scientist: Conducts method development, optimizes MS parameters, and documents trial runs.
  • Mass Spectrometry Specialist: Provides guidance on ion source configuration, tuning, and scan mode settings.
  • QA Officer: Reviews development reports for data integrity and compliance.
  • Head – AMD: Approves the finalized method and development summary.

4. Accountability

The Head of Analytical Method Development is accountable for ensuring the LC-MS methods are scientifically sound, reproducible, and suitable for regulatory or internal use.

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5. Procedure

5.1 Pre-Development Considerations

  1. Review analyte characteristics:
    • Structure, pKa, molecular weight, polarity
    • Known fragmentation patterns or related literature
  2. Check prior analytical methods and determine objective (quantification, impurity profiling, metabolite ID).
  3. Document all pre-development details in Annexure-1: Method Planning Sheet.

5.2 LC System Configuration

  1. Select appropriate LC column (C18, C8, Phenyl, HILIC) based on compound polarity.
  2. Set column dimensions (e.g., 150 mm × 4.6 mm, 3–5 µm) and temperature (25–40°C).
  3. Choose mobile phase combinations (water/acetonitrile or methanol with 0.1% formic acid or ammonium formate).
  4. Perform system suitability on test standards.
  5. Record in Annexure-2: Chromatographic Setup Log.

5.3 Mass Spectrometer Setup

  1. Configure mass spectrometer:
    • Ionization: ESI or APCI
    • Mode: Positive or Negative
    • Polarity switching if required
  2. Infuse analyte to optimize parameters:
    • Capillary voltage
    • Desolvation temperature
    • Gas flow rates (Nebulizer, Drying Gas)
    • Fragmentor and cone voltages
  3. Record MS tuning values in Annexure-3: MS Optimization Record.

5.4 Method Development Trials

  1. Inject test solution and scan in full-scan MS mode (m/z range 100–1000).
  2. Identify molecular ion (M+H)+ or (M-H).
  3. If quantitative, switch to SIM or MRM mode based on:
    • Precursor ion selection
    • Fragment ion optimization
  4. Optimize retention time, peak shape, and resolution.
  5. Document all experimental runs in Annexure-4: Development Trial Sheet.
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5.5 Data Processing and Evaluation

  1. Calculate:
    • Signal-to-noise ratio
    • Retention time consistency
    • Ion suppression or enhancement if matrix involved
  2. Check selectivity using blank, placebo, and spiked sample.
  3. Establish calibration curve and check linearity (5–7 points).
  4. Document observations in Annexure-5: Method Evaluation Summary.

5.6 Final Method Recommendation

  1. Include finalized parameters:
    • Column type and dimensions
    • Mobile phase composition and flow rate
    • Injection volume and temperature
    • Ion source settings and scan type
  2. Submit full method report with system suitability criteria, chromatograms, and spectra.
  3. Obtain QA review and approval from Head – AMD.

6. Abbreviations

  • LC-MS: Liquid Chromatography–Mass Spectrometry
  • SIM: Selected Ion Monitoring
  • MRM: Multiple Reaction Monitoring
  • ESI: Electrospray Ionization
  • APCI: Atmospheric Pressure Chemical Ionization
  • SOP: Standard Operating Procedure

7. Documents

  1. Method Planning Sheet – Annexure-1
  2. Chromatographic Setup Log – Annexure-2
  3. MS Optimization Record – Annexure-3
  4. Development Trial Sheet – Annexure-4
  5. Method Evaluation Summary – Annexure-5

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8. References

  • ICH Q2(R1) – Validation of Analytical Procedures
  • USP <1225> – Validation of Compendial Procedures
  • Instrument Manufacturer’s LC-MS Application Notes

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 Planning Sheet

Analyte Molecular Weight Expected Ion Polarity Purpose
Compound X 332.4 [M+H]+ Positive Impurity Profiling

Annexure-2: Chromatographic Setup Log

Column Mobile Phase A/B Flow Rate Injection Volume
C18, 150×4.6 mm Water/0.1% FA : ACN 0.6 mL/min 10 µL

Annexure-3: MS Optimization Record

Ion Source Mode Capillary Voltage Desolvation Temp
ESI Positive 4000 V 350°C

Annexure-4: Development Trial Sheet

Trial No. Retention Time Peak Area S/N Ratio Comment
1 5.2 min 128934 46 Acceptable

Annexure-5: Method Evaluation Summary

The developed LC-MS method for Compound X showed excellent linearity (r² = 0.9995), precision (RSD < 2%), and detection sensitivity (LOD = 0.5 ng/mL). Finalized parameters were approved for internal qualification studies.

Revision History:

Revision Date Revision No. Details Reason Approved By
04/05/2025 2.0 Incorporated Annexures, MRM selection protocol, tuning log format Annual Review
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