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Orbitrap Ascend Structural Biology Tribrid mass spectrometer

Brochures and specifications | 2024 | Thermo Fisher ScientificInstrumentation
LC/HRMS, LC/MS, LC/MS/MS, LC/Orbitrap
Industries
Proteomics
Manufacturer
Thermo Fisher Scientific

Summary

Importance of the Topic


Structural biology relies on high-resolution mass spectrometry to dissect complex proteins, native assemblies, and post-translational modifications. The ability to scale experimental throughput and extend mass range is crucial for native proteomics, top-down analysis, cross-link mapping, disulfide characterization, and proteoform discovery.

Study Objectives and Overview


This whitepaper presents the Thermo Scientific Orbitrap Ascend Structural Biology Tribrid mass spectrometer and its innovations designed to scale up structural analysis. The focus is on extending quadrupole isolation range, enhancing fragmentation versatility, and automating routine checks to meet diverse structural biology demands.

Methodology


  • Native MS with extended quadrupole isolation (m/z 50–8,000) and DIA-PTCR to simplify spectra and uncover hidden charge states.
  • Top-down fragmentation options (CID, HCD, ETD, EThcD, ETciD, UVPD) for sequence mapping and ligand detection in native membrane proteins.
  • Real-Time Library Search to trigger targeted MSn acquisition and improve cross-linked peptide identification in complex or unenriched samples.
  • EThcD combined with FAIMS Pro Duo interface and microwave-assisted acid hydrolysis for high-confidence disulfide bridge mapping in therapeutic proteins.
  • PTCR MS1 fractionation to resolve high-mass proteoforms above 30 kDa by charge simplification prior to top-down fragmentation.

Used Instrumentation


  • Orbitrap Ascend Structural Biology Tribrid mass spectrometer
  • Advanced active ion beam guide and electrodynamic ion funnel
  • QR5 segmented quadrupole with hyperbolic surfaces
  • Modified dual-pressure linear ion trap (MSn up to 50 Hz)
  • Ultra-High-Field Orbitrap analyzer (>480 K FWHM, up to 45 Hz acquisition)
  • Optional modules: Native MS, PTCR, UVPD, FAIMS Pro Duo interface
  • Auto-Ready ion source for automated and schedulable calibrations

Key Results and Discussion


  • DIA-PTCR deconvolution of nanodisc assemblies (~140–175 kDa) revealed precise lipid stoichiometries.
  • Native top-down workflows delivered high sequence coverage and identified hidden ligands in membrane protein complexes.
  • Real-Time Library Search doubled cross-link identifications in HeLa samples, enhancing throughput and confidence.
  • EThcD with FAIMS Pro Duo achieved rapid, detailed mapping of antibody disulfide bonds with low background noise.
  • PTCR fractionation expanded proteoform detection in HEK293 cell extracts, identifying species above 30 kDa with ProSightPD software.

Benefits and Practical Applications


The platform streamlines structural characterization across workflows, offering higher throughput, extended mass coverage, and versatile fragmentation. It supports native proteomics, top-down projects, cross-linking studies, disulfide analysis, and proteoform profiling, aiding research, QA/QC, and pharmaceutical development.

Future Trends and Opportunities


Integration of AI-driven acquisition methods, enhanced ion mobility separations, and real-time data analytics will further accelerate structural proteomics. Emerging areas include high-throughput QC pipelines, in situ complex assembly analysis, and multi-omic integration for systems-level insights.

Conclusion


The Orbitrap Ascend Structural Biology Tribrid mass spectrometer advances the scale, versatility, and automation of structural analysis, enabling comprehensive insights into proteins and complexes and setting a new benchmark for structural proteomics workflows.

Content was automatically generated from an orignal PDF document using AI and may contain inaccuracies.

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