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First-Principles Collision Cross Section Measurements of Large Proteins and Protein Complexes. | LitMetric

AI Article Synopsis

  • The study reports on rotationally averaged collision cross section (CCS) values for various proteins and complexes, using a highly sensitive mass spectrometer specifically designed for this purpose.
  • It finds that experimental CCS values closely match previously published data, with a consistency of about 5.5%.
  • The research highlights the significance of ion mobility resolution in analyzing large biomolecules, revealing how it can help in understanding protein complexities related to factors like post-translational modifications and conformational changes.

Article Abstract

Rotationally averaged collision cross section (CCS) values for a series of proteins and protein complexes ranging in size from 8.6 to 810 kDa are reported. The CCSs were obtained using a native electrospray ionization drift tube ion mobility-Orbitrap mass spectrometer specifically designed to enhance sensitivity while having high-resolution ion mobility and mass capabilities. Periodic focusing (PF)-drift tube (DT)-ion mobility (IM) provides first-principles determination of the CCS of large biomolecules that can then be used as CCS calibrants. The experimental, first-principles CCS values are compared to previously reported experimentally determined and computationally calculated CCS using projected superposition approximation (PSA), the Ion Mobility Projection Approximation Calculation Tool (IMPACT), and Collidoscope. Experimental CCS values are generally in agreement with previously reported CCSs, with values falling within ∼5.5%. In addition, an ion mobility resolution (CCS centroid divided by CCS fwhm) of ∼60 is obtained for pyruvate kinase (MW ∼ 233 kDa); however, ion mobility resolution for bovine serum albumin (MW ∼ 68 kDa) is less than ∼20, which arises from sample impurities and underscores the importance of sample quality. The high resolution afforded by the ion mobility-Orbitrap mass analyzer provides new opportunities to understand the intricate details of protein complexes such as the impact of post-translational modifications (PTMs), stoichiometry, and conformational changes induced by ligand binding.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7967297PMC
http://dx.doi.org/10.1021/acs.analchem.0c01285DOI Listing

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