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Simplifying CE-SDS Data Processing

Technical notes | 2018 | SCIEXInstrumentation
Capillary electrophoresis
Industries
Manufacturer
SCIEX

Summary

Significance of the Topic


Capillary electrophoresis–SDS (CE-SDS) is a key technique for fragment analysis of monoclonal antibodies and large biologics. Consistent peak migration times are essential for reliable quantitation, yet buffer evaporation can cause drift and complicate data analysis.

Objectives and Study Overview


This collaboration between MedImmune and SCIEX investigated whether layering mineral oil over gel buffer vials could prevent evaporation-induced drift. The study assessed assay accuracy, precision, linearity, autosampler stability, and limits of detection and quantitation under reducing and non-reducing conditions.

Methodology and Instrumentation


  • System: SCIEX PA 800 Plus Pharmaceutical Analysis System
  • Capillary: 20 cm effective length, 50 µm ID fused silica (EZ-CE Cartridge)
  • Buffers: HR separation gel buffer; Gel-R buffer with or without mineral oil overlay
  • Sample prep: NIST mAb at 1.0 mg/mL with 10 kDa internal standard, reduced with β-mercaptoethanol or non-reduced with iodoacetamide; stressed by incubation at 67 °C for 24 h
  • Electrophoresis: 15 kV at 25 °C, reversed polarity, 1 kV injection for 40 s, 54 min run time
  • Detection: PDA at 214 nm; data acquired with 32 Karat software and processed in Empower

Key Findings and Discussion


  • Mineral oil overlay virtually eliminated drift in migration times, reducing peak shifts from over 1 min to under 0.2 min across a run.
  • Assay accuracy and precision were maintained, with CVs below 0.2% and purity results consistent within 1% differential.
  • Linearity remained strong (R² ≥ 0.98) and LOD/LOQ values (LOQ: 0.13–0.21% TCA; LOD: 0.04–0.07% TCA) were unaffected by oil use.
  • Autosampler stability over 60 h showed no drift when mineral oil was applied, preserving peak resolution over extended sequences.

Benefits and Practical Applications


The simple addition of mineral oil to Gel-R vials delivers more reproducible CE-SDS profiles, reduces manual data correction, and allows tighter integration windows. This enhances throughput and reliability in biopharmaceutical QC, comparability studies, and stability testing.

Future Trends and Potential Applications


  • Automation of mineral oil dispensing for standardized buffer preparation.
  • Application of this evaporation-control approach to other electrophoretic platforms and buffer systems.
  • Integration with software-based real-time drift correction and advanced data analytics for further workflow optimization.

Conclusion


Layering mineral oil on gel buffer vials during CE-SDS assay setup effectively prevents evaporation-induced migration time drift without impacting performance metrics. This straightforward modification enhances data consistency and streamlines analytical workflows for monoclonal antibody characterization.

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