Inhibiting Mycobacterium tuberculosis CoaBC by targeting an allosteric site

Mendes, Vitor; Green, Simon R.; Evans, Joanna C.; Hess, Jeannine; Blaszczyk, Michal; Spry, Christina; Bryant, Owain; Cory-Wright, James; Chan, Daniel S-H.; Torres, Pedro H. M.; Wang, Zhe; Nahiyaan, Navid; O’Neill, Sandra; Damerow, Sebastian; Post, John; Bayliss, Tracy; Lynch, Sasha L.; Coyne, Anthony G.; Ray, Peter C.; Abell, Chris; Rhee, Kyu Y.; Boshoff, Helena I. M.; Barry, Clifton E.; Mizrahi, Valerie; Wyatt, Paul G.; Blundell, Tom L.

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Authors

Mendes, Vitor

Green, Simon R.

Evans, Joanna C.

Hess, Jeannine

Blaszczyk, Michal

Spry, Christina

Bryant, Owain

Publication Date

2021-01-08

Journal Title

Nature Communications

Publisher

Nature Publishing Group UK

Volume

Issue

Language

Type

Article

This Version

VoR

Metadata

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Citation

Mendes, V., Green, S. R., Evans, J. C., Hess, J., Blaszczyk, M., Spry, C., Bryant, O., et al. (2021). Inhibiting Mycobacterium tuberculosis CoaBC by targeting an allosteric site. Nature Communications, 12 (1)https://doi.org/10.1038/s41467-020-20224-x

Description

Funder: Bill and Melinda Gates Foundation (Bill & Melinda Gates Foundation)

Abstract

Abstract: Coenzyme A (CoA) is a fundamental co-factor for all life, involved in numerous metabolic pathways and cellular processes, and its biosynthetic pathway has raised substantial interest as a drug target against multiple pathogens including Mycobacterium tuberculosis. The biosynthesis of CoA is performed in five steps, with the second and third steps being catalysed in the vast majority of prokaryotes, including M. tuberculosis, by a single bifunctional protein, CoaBC. Depletion of CoaBC was found to be bactericidal in M. tuberculosis. Here we report the first structure of a full-length CoaBC, from the model organism Mycobacterium smegmatis, describe how it is organised as a dodecamer and regulated by CoA thioesters. A high-throughput biochemical screen focusing on CoaB identified two inhibitors with different chemical scaffolds. Hit expansion led to the discovery of potent and selective inhibitors of M. tuberculosis CoaB, which we show to bind to a cryptic allosteric site within CoaB.

Keywords

Article, /631/45/607, /631/154, /631/535/1266, /82/83, /145, /45/41, /49/98, article

Sponsorship

Bill and Melinda Gates Foundation (Bill & Melinda Gates Foundation) (OPP1024021, OPP1158806, OPP1024021, OPP1024021, OPP1158806)

Department of Health | National Health and Medical Research Council (NHMRC) (1016357)

Wellcome Trust (Wellcome) (200814_Z_16_Z)

Identifiers

s41467-020-20224-x, 20224

External DOI: https://doi.org/10.1038/s41467-020-20224-x

This record's URL: https://www.repository.cam.ac.uk/handle/1810/315925

Rights

Attribution 4.0 International (CC BY 4.0)

Licence URL: https://creativecommons.org/licenses/by/4.0/

Except where otherwise noted, this item's licence is described as Attribution 4.0 International (CC BY 4.0)