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Unveiling hidden protein depths: a high-throughput plasma proteomics workflow for enhanced biomarker discovery on Orbitrap Astral MS

Posters | 2024 | Thermo Fisher Scientific | HUPOInstrumentation
LC/MS, LC/Orbitrap, LC/HRMS, LC/MS/MS
Industries
Proteomics , Clinical Research
Manufacturer
Thermo Fisher Scientific

Summary

Importance of the Topic


Blood plasma is a rich source of potential biomarkers for early disease detection due to its non-invasive collection and complex proteome composition. However, the wide dynamic range of plasma proteins poses challenges for comprehensive analysis. Integrating high-resolution mass spectrometry with advanced sample preparation strategies is crucial to revealing low-abundance proteins and supporting translational biomarker research.

Objectives and Study Overview


  • Develop robust high-throughput plasma proteomics workflows combining varied sample preparation techniques.
  • Compare neat plasma, nanoparticle-based enrichment (Proteograph XT), and immunodepletion of abundant proteins.
  • Assess performance across multiple LC–MS throughputs (100, 60, 24, 16 samples/day) using label-free DIA on the Orbitrap Astral MS.

Methodology and Instrumentation


The study employed pooled healthy donor plasma processed in three ways: direct digest (neat), nanoparticle enrichment via Seer Proteograph XT, and depletion of top-14 abundant proteins using high-select spin columns. After trypsin/Lys-C digestion, peptides were separated on various columns (15 cm, 50 cm EASY-Spray PepMap; 60 cm IonOpticks) and resolved on a Vanquish Neo UHPLC system. The Orbitrap Astral MS operated in DIA mode enabled comprehensive protein quantitation. Data were analyzed with Spectronaut, DIA-NN, and Proteome Discoverer with CHIMERYS.

Key Results and Discussion


  • Deep proteome coverage: Over 4,000, 5,000, 6,000, and 8,000 protein groups identified at 100, 60, 24, and 16 samples/day, respectively, with CVs of 4–6%.
  • Neat plasma workflow yielded ~720 proteins at 60 SPD (CV ~6%), balancing simplicity and throughput.
  • Top-14 depletion improved coverage to 1,100–1,850 proteins (100–24 SPD) with CVs around 10%.
  • Proteograph XT enrichment identified ~3,900–4,900 proteins at 100–60 SPD (CV ~6%), delivering the deepest automated workflow.
  • Incorporating a spectral library expanded identifications by 300–600 proteins in high-throughput runs.
  • Complementarity observed: ~20–25% of depletion-unique proteins were not captured by enrichment, supporting combined approaches.

Benefits and Practical Applications


  • Scalable workflows tailored to study size and depth requirements.
  • High precision (CV <6%) ensures reliable quantitation in large cohorts.
  • Automated sample preparation and rapid DIA acquisition accelerate biomarker discovery pipelines.
  • Flexible instrument configurations enable laboratories to optimize throughput versus depth.

Future Trends and Opportunities


Advancements in spectral library generation, AI-driven data analysis, and further optimization of sample preparation will enhance sensitivity and proteome coverage. Integration with multi-omics platforms and expansion to clinical cohorts promises to advance personalized diagnostics and therapeutic monitoring.

Conclusion


The presented high-throughput plasma proteomics workflows, leveraging Orbitrap Astral MS and varied preparation strategies, achieve unmatched depth and reproducibility. These methods empower large-scale biomarker studies and support translational research by uncovering low-abundance proteins in complex plasma samples.

References


  • Yang K., Flora A., Motamedchaboki K., et al. Unveiling hidden protein depths: a high-throughput plasma proteomics workflow for enhanced biomarker discovery on Orbitrap Astral MS. Thermo Fisher Scientific Application Note PO147-2024-EN.
  • Spectronaut, Biognosys AG.
  • CHIMERYS intelligent search algorithm, MSAID.

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