A Preclinical Candidate Targeting Mycobacterium tuberculosis KasA

Daigo Inoyama,Divya Awasthi,Glenn C. Capodagli,Kholiswa Tsotetsi,Paridhi Sukheja,Matthew D. Zimmerman,Shao-Gang Li,Ravindra Jadhav,Riccardo Russo,Xin Wang,Courtney Grady,Todd Richmann,Riju Shrestha,Liping Li,Yong Mo Ahn,Hsin-pin Ho Liang,Marizel Mina,Steven Park,David S. Perlin,Nancy D. Connell,Véronique Dartois,David Alland,Matthew B. Neiditch,Pradeep Kumar,Joel S. Freundlich

A Preclinical Candidate Targeting Mycobacterium tuberculosis KasA

2020

Summary Published Mycobacterium tuberculosis β-ketoacyl-ACP synthase KasA inhibitors lack sufficient potency and/or pharmacokinetic properties. A structure-based approach was used to optimize existing KasA inhibitor DG167. This afforded indazole JSF-3285 with a 30-fold increase in mouse plasma exposure. Biochemical, genetic, and X-ray studies confirmed JSF-3285 targets KasA. JSF-3285 offers substantial activity in an acute mouse model of infection and in the corresponding chronic infection model, with efficacious reductions in colony-forming units at doses as low as 5 mg/kg once daily orally and improvement of the efficacy of front-line drugs isoniazid or rifampicin. JSF-3285 is a promising preclinical candidate for tuberculosis.

Keywords:

Isoniazid
Indazole
plasma exposure
Potency
Molecular biology
Mycobacterium tuberculosis
Tuberculosis
Rifampicin
Pharmacology
Biology
Pharmacokinetics
once daily
chronic infection

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