Distinguishing Protein Chemical Topologies Using Supercharging Ion Mobility Spectrometry‐Mass Spectrometry

Author:

Lee Jiyeon1,Im Dahye1,Liu Yajie2,Fang Jing2,Tian Xibao2,Kim Minsu1,Zhang Wen‐Bin2ORCID,Seo Jongcheol1ORCID

Affiliation:

1. Department of Chemistry Pohang University of Science and Technology (POSTECH) 77 Cheongam-ro, Nam-gu Pohang 37673 Gyeonsangbuk-do (Republic of Korea

2. Beijing National Laboratory for Molecular Sciences Key Laboratory of Polymer Chemistry & Physics of Ministry of Education Center for Soft Matter Science and Engineering College of Chemistry and Molecular Engineering Peking University Beijing 100871 P. R. China

Abstract

AbstractA technique combining ion mobility spectrometry‐mass spectrometry (IMS‐MS) and supercharging electrospray ionization (ESI) has been demonstrated to differentiate protein chemical topology effectively. Incorporating as many charges as possible into proteins via supercharging ESI allows the protein chains to be largely unfolded and stretched, revealing their hidden chemical topology. Different chemical topologies result in differing geometrical sizes of the unfolded proteins due to constraints in torsional rotations in cyclic domains. By introducing new topological indices, such as the chain‐length‐normalized collision cross‐section (CCS) and the maximum charge state (zM) in the extensively unfolded state, we were able to successfully differentiate various protein chemical topologies, including linear chains, ring‐containing topologies (lasso, tadpole, multicyclics, etc.), and mechanically interlocked rings, like catenanes.

Funder

National Natural Science Foundation of China

Key Technologies Research and Development Program

Publisher

Wiley

Subject

General Medicine

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