Literature DB >> 31939065

Targeting the menaquinol binding loop of mycobacterial cytochrome bd oxidase.

Amaravadhi Harikishore1, Sherilyn Shi Min Chong1,2,3, Priya Ragunathan2, Roderick W Bates1, Gerhard Grüber4.   

Abstract

Mycobacteria have shown enormous resilience to survive and persist by remodeling and altering metabolic requirements. Under stringent conditions or exposure to drugs, mycobacteria have adapted to rescue themselves by shutting down their major metabolic activity and elevate certain survival factor levels and efflux pathways to survive and evade the effects of drug treatments. A fundamental feature in this adaptation is the ability of mycobacteria to vary the enzyme composition of the electron transport chain (ETC), which generates the proton motive force for the synthesis of adenosine triphosphate via oxidative phosphorylation. Mycobacteria harbor dehydrogenases to fuel the ETC, and two terminal respiratory oxidases, an aa3-type cytochrome c oxidase (cyt-bcc-aa3) and a bacterial specific cytochrome bd-type menaquinol oxidase (cyt-bd). In this study, we employed homology modeling and structure-based virtual screening studies to target mycobacteria-specific residues anchoring the b558 menaquinol binding region of Mycobacterium tuberculosis cyt-bd oxidase to obtain a focused library. Furthermore, ATP synthesis inhibition assays were carried out. One of the ligands MQL-H2 inhibited both NADH2- and succinate-driven ATP synthesis inhibition of Mycobacterium smegmatis inside-out vesicles in micromolar potency. Similarly, MQL-H2 also inhibited NADH2-driven ATP synthesis in inside-out vesicles of the cytochrome-bcc oxidase deficient M. smegmatis strain. Since neither varying the electron donor substrates nor deletion of the cyt-bcc oxidase, a major source of protons, hindered the inhibitory effects of the MQL-H2, reflecting that MQL-H2 targets the terminal oxidase cytochrome bd oxidase, which was consistent with molecular docking studies. Characterization of novel cytochrome bd oxidase Menaquinol binding domain inhibitor (MQL-H2) using virtual screening and ATP synthesis inhibition assays.

Entities:  

Keywords:  Cytochrome bd oxidase; Drug resistance; Mycobacteria; OXPHOS pathway; Respiration; Tuberculosis

Year:  2020        PMID: 31939065     DOI: 10.1007/s11030-020-10034-0

Source DB:  PubMed          Journal:  Mol Divers        ISSN: 1381-1991            Impact factor:   2.943


  25 in total

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3.  Glutamate 107 in subunit I of the cytochrome bd quinol oxidase from Escherichia coli is protonated and near the heme d/heme b595 binuclear center.

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4.  Clofazimine for the treatment of multidrug-resistant tuberculosis: prospective, multicenter, randomized controlled study in China.

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Journal:  Clin Infect Dis       Date:  2015-01-20       Impact factor: 9.079

5.  Hypoxia-activated cytochrome bd expression in Mycobacterium smegmatis is cyclic AMP receptor protein dependent.

Authors:  Htin Lin Aung; Michael Berney; Gregory M Cook
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6.  Structure of a bd oxidase indicates similar mechanisms for membrane-integrated oxygen reductases.

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9.  Structure-activity relationships for unit C pyridyl analogues of the tuberculosis drug bedaquiline.

Authors:  Adrian Blaser; Hamish S Sutherland; Amy S T Tong; Peter J Choi; Daniel Conole; Scott G Franzblau; Christopher B Cooper; Anna M Upton; Manisha Lotlikar; William A Denny; Brian D Palmer
Journal:  Bioorg Med Chem       Date:  2019-02-15       Impact factor: 3.641

10.  Structure-activity relationships for analogs of the tuberculosis drug bedaquiline with the naphthalene unit replaced by bicyclic heterocycles.

Authors:  Hamish S Sutherland; Amy S T Tong; Peter J Choi; Daniel Conole; Adrian Blaser; Scott G Franzblau; Christopher B Cooper; Anna M Upton; Manisha U Lotlikar; William A Denny; Brian D Palmer
Journal:  Bioorg Med Chem       Date:  2018-02-20       Impact factor: 3.641

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5.  Synthesis and Biological Screening of New Lawson Derivatives as Selective Substrate-Based Inhibitors of Cytochrome bo3 Ubiquinol Oxidase from Escherichia coli.

Authors:  Isam Elamri; Melanie Radloff; Katharina F Hohmann; Vijaykumar D Nimbarte; Hamid R Nasiri; Michael Bolte; Schara Safarian; Hartmut Michel; Harald Schwalbe
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Review 6.  Recent Advances in Structural Studies of Cytochrome bd and Its Potential Application as a Drug Target.

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  6 in total

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