Structure-based design of MptpB inhibitors that reduce multi-drug-resistant mycobacterium tuberculosis survival and infection burden in vivo

Vickers, Clare F.
Silva, Ana P. G.
Chakraborty, Ajanta
Fernandez, Paulina
Kurepina, Natalia
Saville, Charis
Naranjo, Yandi
Pons Vallès, Miquel
Schnettger, Laura S.
Gutierrez, Maximiliano G.
Park, Steven
Keiswirth, Barry N.
Perlin, David S.
Thomas, Eric J.
Cavet, Jennifer S.
Tabernero, Lydia

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Publication date

July 2019

DOI

10.1021/acs.jmedchem.8b00832

Publisher

American Chemical Society (ACS)

Journal

Journal of Medicinal Chemistry

Abstract

Mycobacterium tuberculosis protein-tyrosine-phosphatase B (MptpB) is a secreted virulence factor that subverts antimicrobial activity in the host. We report here the structure-based design of selective MptpB inhibitors that reduce survival of multidrug-resistant tuberculosis strains in macrophages and enhance killing efficacy by first-line antibiotics. Monotherapy with an orally bioavailable MptpB inhibitor reduces infection burden in acute and chronic guinea pig models and improves the overall pathology. Our findings provide a new paradigm for tuberculosis treatmen

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Structure-based design of MptpB inhibitors that reduce multi-drug-resistant mycobacterium tuberculosis survival and infection burden in vivo

Abstract

Extracted data

Structure-based design of MptpB inhibitors that reduce multi-drug-resistant mycobacterium tuberculosis survival and infection burden in vivo

Abstract

Extracted data

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