Implications of Binding Mode and Active Site Flexibility for Inhibitor Potency against the Salicylate Synthase from Mycobacterium tuberculosis

Chi, Gamma; Manos-Turvey, Alexandra; O’Connor, Patrick D.; Johnston, Jodie M.; Evans, Genevieve L.; Baker, Edward N.; Payne, Richard J.; Lott, J. Shaun; Bulloch, Esther M. M.

doi:10.1021/bi3002067

Article (Scientific journals)

Implications of Binding Mode and Active Site Flexibility for Inhibitor Potency against the Salicylate Synthase from Mycobacterium tuberculosis

Chi, Gamma; Manos-Turvey, Alexandra; O’Connor, Patrick D. et al.

2012 • In Biochemistry, 51 (24), p. 4868-4879

Peer Reviewed verified by ORBi

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https://hdl.handle.net/2268/197826

DOI
10.1021/bi3002067

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22607697

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Abstract :

[en] MbtI is the salicylate synthase that catalyzes the first committed step in the synthesis of the iron chelating compound mycobactin in Mycobacterium tuberculosis. We previously developed a series of aromatic inhibitors against MbtI based on the reaction intermediate for this enzyme, isochorismate. The most potent of these inhibitors had hydrophobic substituents, ranging in size from a methyl to a phenyl group, appended to the terminal alkene of the enolpyruvyl group. These compounds exhibited low micromolar inhibition constants against MbtI and were at least an order of magnitude more potent than the parental compound for the series, which carries a native enolpyruvyl group. In this study, we sought to understand how the substituted enolpyruvyl group confers greater potency, by determining cocrystal structures of MbtI with six inhibitors from the series. A switch in binding mode at the MbtI active site is observed for inhibitors carrying a substituted enolpyruvyl group, relative to the parental compound. Computational studies suggest that the change in binding mode, and higher potency, is due to the effect of the substituents on the conformational landscape of the core inhibitor structure. The crystal structures and fluorescence-based thermal shift assays indicate that substituents larger than a methyl group are accommodated in the MbtI active site through significant but localized flexibility in the peptide backbone. These findings have implications for the design of improved inhibitors of MbtI, as well as other chorismate-utilizing enzymes from this family.

Disciplines :

Biochemistry, biophysics & molecular biology

Author, co-author :

Chi, Gamma

Manos-Turvey, Alexandra ; University of Sydney > School of Chemistry

O’Connor, Patrick D.

Johnston, Jodie M.

Evans, Genevieve L.

Baker, Edward N.

Payne, Richard J.

Lott, J. Shaun

Bulloch, Esther M. M.

Language :

English

Title :

Implications of Binding Mode and Active Site Flexibility for Inhibitor Potency against the Salicylate Synthase from Mycobacterium tuberculosis

Publication date :

2012

Journal title :

Biochemistry

ISSN :

0006-2960

eISSN :

1520-4995

Publisher :

American Chemical Society, Washington, United States - District of Columbia

Volume :

Issue :

Pages :

4868-4879

Peer reviewed :

Peer Reviewed verified by ORBi

Additional URL :

http://dx.doi.org/10.1021/bi3002067

Available on ORBi :

since 03 June 2016

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