A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR

Abdalkarim Tanina; Alexandre Wohlkönig; Sameh H. Soror; Marion Flipo; Baptiste Villemagne; Hugues Prevet; Benoit Déprez; Martin Moune; Hélène Perée; Franck Meyer; Alain R. Baulard; Nicolas Willand; René Wintjens

doi:10.1016/j.bbapap.2018.12.003

A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR

Abdalkarim Tanina, Alexandre Wohlkönig, Sameh H. Soror, Marion Flipo, Baptiste Villemagne, Hugues Prevet, Benoit Déprez, Martin Moune, Hélène Perée, Franck Meyer, Alain R. Baulard, Nicolas Willand, René Wintjens

Research output: Contribution to journal › Article › peer-review

12 Citations (Scopus)

Abstract

The Mycobacterium tuberculosis EthR is a member of the TetR family of repressors, controlling the expression of EthA, a mono-oxygenase responsible for the bioactivation of the prodrug ethionamide. This protein was established as a promising therapeutic target against tuberculosis, allowing, when inhibited by a drug-like molecule, to boost the action of ethionamide. Dozens of EthR crystal structures have been solved in complex with ligands. Herein, we disclose EthR structures in complex with 18 different small molecules and then performed in-depth analysis on the complete set of EthR structures that provides insights on EthR-ligand interactions. The 81 molecules solved in complex with EthR show a large diversity of chemical structures that were split up into several chemical clusters. Two of the most striking common points of EthR-ligand interactions are the quasi-omnipresence of a hydrogen bond bridging compounds with Asn179 and the high occurrence of π-π interactions involving Phe110. A systematic analysis of the protein-ligand contacts identified eight hot spot residues that defined the basic structural features governing the binding mode of small molecules to EthR. Implications for the design of new potent inhibitors are discussed.

Original language	English
Pages (from-to)	248-258
Number of pages	11
Journal	Biochimica et Biophysica Acta - Proteins and Proteomics
Volume	1867
Issue number	3
DOIs	https://doi.org/10.1016/j.bbapap.2018.12.003
Publication status	Published - 1 Mar 2019

Keywords

Binding interaction
Drug design
Ethionamide
Small molecule
Tuberculosis
X-ray crystallography

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10.1016/j.bbapap.2018.12.003

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Tanina, A., Wohlkönig, A., Soror, S. H., Flipo, M., Villemagne, B., Prevet, H., Déprez, B., Moune, M., Perée, H., Meyer, F., Baulard, A. R., Willand, N., & Wintjens, R. (2019). A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR. Biochimica et Biophysica Acta - Proteins and Proteomics, 1867(3), 248-258. https://doi.org/10.1016/j.bbapap.2018.12.003

Tanina, Abdalkarim ; Wohlkönig, Alexandre ; Soror, Sameh H. ; Flipo, Marion ; Villemagne, Baptiste ; Prevet, Hugues ; Déprez, Benoit ; Moune, Martin ; Perée, Hélène ; Meyer, Franck ; Baulard, Alain R. ; Willand, Nicolas ; Wintjens, René. / A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR. In: Biochimica et Biophysica Acta - Proteins and Proteomics. 2019 ; Vol. 1867, No. 3. pp. 248-258.

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title = "A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR",

abstract = "The Mycobacterium tuberculosis EthR is a member of the TetR family of repressors, controlling the expression of EthA, a mono-oxygenase responsible for the bioactivation of the prodrug ethionamide. This protein was established as a promising therapeutic target against tuberculosis, allowing, when inhibited by a drug-like molecule, to boost the action of ethionamide. Dozens of EthR crystal structures have been solved in complex with ligands. Herein, we disclose EthR structures in complex with 18 different small molecules and then performed in-depth analysis on the complete set of EthR structures that provides insights on EthR-ligand interactions. The 81 molecules solved in complex with EthR show a large diversity of chemical structures that were split up into several chemical clusters. Two of the most striking common points of EthR-ligand interactions are the quasi-omnipresence of a hydrogen bond bridging compounds with Asn179 and the high occurrence of π-π interactions involving Phe110. A systematic analysis of the protein-ligand contacts identified eight hot spot residues that defined the basic structural features governing the binding mode of small molecules to EthR. Implications for the design of new potent inhibitors are discussed.",

keywords = "Binding interaction, Drug design, Ethionamide, Small molecule, Tuberculosis, X-ray crystallography",

author = "Abdalkarim Tanina and Alexandre Wohlk{\"o}nig and Soror, {Sameh H.} and Marion Flipo and Baptiste Villemagne and Hugues Prevet and Benoit D{\'e}prez and Martin Moune and H{\'e}l{\`e}ne Per{\'e}e and Franck Meyer and Baulard, {Alain R.} and Nicolas Willand and Ren{\'e} Wintjens",

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day = "1",

doi = "10.1016/j.bbapap.2018.12.003",

language = "English",

volume = "1867",

pages = "248--258",

journal = "Biochimica et Biophysica Acta - Proteins and Proteomics",

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Tanina, A, Wohlkönig, A, Soror, SH, Flipo, M, Villemagne, B, Prevet, H, Déprez, B, Moune, M, Perée, H, Meyer, F, Baulard, AR, Willand, N & Wintjens, R 2019, 'A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR', Biochimica et Biophysica Acta - Proteins and Proteomics, vol. 1867, no. 3, pp. 248-258. https://doi.org/10.1016/j.bbapap.2018.12.003

A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR. / Tanina, Abdalkarim; Wohlkönig, Alexandre; Soror, Sameh H.; Flipo, Marion; Villemagne, Baptiste; Prevet, Hugues; Déprez, Benoit; Moune, Martin; Perée, Hélène; Meyer, Franck; Baulard, Alain R.; Willand, Nicolas; Wintjens, René.

In: Biochimica et Biophysica Acta - Proteins and Proteomics, Vol. 1867, No. 3, 01.03.2019, p. 248-258.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR

AU - Tanina, Abdalkarim

AU - Wohlkönig, Alexandre

AU - Soror, Sameh H.

AU - Flipo, Marion

AU - Villemagne, Baptiste

AU - Prevet, Hugues

AU - Déprez, Benoit

AU - Moune, Martin

AU - Perée, Hélène

AU - Meyer, Franck

AU - Baulard, Alain R.

AU - Willand, Nicolas

AU - Wintjens, René

PY - 2019/3/1

Y1 - 2019/3/1

N2 - The Mycobacterium tuberculosis EthR is a member of the TetR family of repressors, controlling the expression of EthA, a mono-oxygenase responsible for the bioactivation of the prodrug ethionamide. This protein was established as a promising therapeutic target against tuberculosis, allowing, when inhibited by a drug-like molecule, to boost the action of ethionamide. Dozens of EthR crystal structures have been solved in complex with ligands. Herein, we disclose EthR structures in complex with 18 different small molecules and then performed in-depth analysis on the complete set of EthR structures that provides insights on EthR-ligand interactions. The 81 molecules solved in complex with EthR show a large diversity of chemical structures that were split up into several chemical clusters. Two of the most striking common points of EthR-ligand interactions are the quasi-omnipresence of a hydrogen bond bridging compounds with Asn179 and the high occurrence of π-π interactions involving Phe110. A systematic analysis of the protein-ligand contacts identified eight hot spot residues that defined the basic structural features governing the binding mode of small molecules to EthR. Implications for the design of new potent inhibitors are discussed.

AB - The Mycobacterium tuberculosis EthR is a member of the TetR family of repressors, controlling the expression of EthA, a mono-oxygenase responsible for the bioactivation of the prodrug ethionamide. This protein was established as a promising therapeutic target against tuberculosis, allowing, when inhibited by a drug-like molecule, to boost the action of ethionamide. Dozens of EthR crystal structures have been solved in complex with ligands. Herein, we disclose EthR structures in complex with 18 different small molecules and then performed in-depth analysis on the complete set of EthR structures that provides insights on EthR-ligand interactions. The 81 molecules solved in complex with EthR show a large diversity of chemical structures that were split up into several chemical clusters. Two of the most striking common points of EthR-ligand interactions are the quasi-omnipresence of a hydrogen bond bridging compounds with Asn179 and the high occurrence of π-π interactions involving Phe110. A systematic analysis of the protein-ligand contacts identified eight hot spot residues that defined the basic structural features governing the binding mode of small molecules to EthR. Implications for the design of new potent inhibitors are discussed.

KW - Binding interaction

KW - Drug design

KW - Ethionamide

KW - Small molecule

KW - Tuberculosis

KW - X-ray crystallography

UR - http://www.mendeley.com/research/comprehensive-analysis-proteinligand-interactions-crystal-structures-mycobacterium-tuberculosis-ethr

U2 - 10.1016/j.bbapap.2018.12.003

DO - 10.1016/j.bbapap.2018.12.003

M3 - Article

VL - 1867

SP - 248

EP - 258

JO - Biochimica et Biophysica Acta - Proteins and Proteomics

JF - Biochimica et Biophysica Acta - Proteins and Proteomics

SN - 1570-9639

IS - 3

ER -

A comprehensive analysis of the protein-ligand interactions in crystal structures of Mycobacterium tuberculosis EthR

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