Cofactor Editing by the G-protein Metallochaperone Domain Regulates the Radical B 12 Enzyme IcmF

Zhu, Li, University of Michigan; Kenichi, Kitanishi, University of Michigan; Umar T., Twahir, Emory University; Valentin, Cracan, University of Michigan; Derrell, Chapman, University of Michigan; Kurt, Warncke, Emory University; Ruma, Banerjee, University of Michigan

Persistent URL

https://open.library.emory.edu/purl/81937pvmmd-emory

Last modified

02/20/2025

Type of Material

Article

Authors

Zhu Li, University of Michigan

Kenichi Kitanishi, University of Michigan

Umar T. Twahir, Emory University

Valentin Cracan, University of Michigan

Derrell Chapman, University of Michigan

Kurt Warncke, Emory UniversityRuma Banerjee, University of Michigan

Language

English

Date

2017-03-10

Publisher

American Society for Biochemistry and Molecular Biology

Publication Version

Final Published Version

Copyright Statement

© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

Final Published Version (URL)

http://dx.doi.org/10.1074/jbc.M117.775957

Title of Journal or Parent Work

Journal of Biological Chemistry

ISSN

0021-9258

Volume

292

Issue

10

Start Page

3977

End Page

3987

Grant/Funding Information

This work was supported in part by National Institutes of Health Grant DK45776.

Abstract

IcmF is a 5′-deoxyadenosylcobalamin (AdoCbl)-dependent enzyme that catalyzes the carbon skeleton rearrangement of isobutyryl-CoA to butyryl-CoA. It is a bifunctional protein resulting from the fusion of a G-protein chaperone with GTPase activity and the cofactor- and substrate-binding mutase domains with isomerase activity. IcmF is prone to inactivation during catalytic turnover, thus setting up its dependence on a cofactor repair system. Herein, we demonstrate that the GTPase activity of IcmF powers the ejection of the inactive cob(II)alamin cofactor and requires the presence of an acceptor protein, adenosyltransferase, for receiving it. Adenosyltransferase in turn converts cob(II)alamin to AdoCbl in the presence of ATP and a reductant. The repaired cofactor is then reloaded onto IcmF in a GTPase-gated step. The mechanistic details of cofactor loading and offloading from the AdoCbl-dependent IcmF are distinct from those of the better characterized and homologous methylmalonyl-CoA mutase/G-protein chaperone system.

Author Notes

Corresponding Author: Ruma Banerjee Tel.: Phone: 734-615-5238; E-mail:rbanerje@umich.edu

Keywords

Research Categories

Biology, Molecular
Physics, General

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Cofactor Editing by the G-protein Metallochaperone Domain Regulates the Radical B 12 Enzyme IcmF

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