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1,4-Azaindole,a Potential Drug Candidate for Treatment of Tuberculosis
Authors:Monalisa Chatterji  Radha Shandil  M. R. Manjunatha  Suresh Solapure  Vasanthi Ramachandran  Naveen Kumar  Ramanatha Saralaya  Vijender Panduga  Jitendar Reddy  Prabhakar KR  Sreevalli Sharma  Claire Sadler  Christopher B. Cooper  Khisi Mdluli  Pravin S. Iyer  Shridhar Narayanan  Pravin S. Shirude
Affiliation:aDepartment of Biosciences, IMED Infection, AstraZeneca, Bangalore, India;bDMPK and Animal Sciences, IMED Infection, AstraZeneca, Bangalore, India;cDepartment of Medicinal Chemistry, IMED Infection, AstraZeneca, Bangalore, India;dSafety Assessment, IMED, AstraZeneca, Alderly Park, Mereside, United Kingdom;eGlobal Alliance for TB Drug Development, New York, New York, USA
Abstract:New therapeutic strategies against multidrug-resistant (MDR) and extensively drug-resistant (XDR) Mycobacterium tuberculosis are urgently required to combat the global tuberculosis (TB) threat. Toward this end, we previously reported the identification of 1,4-azaindoles, a promising class of compounds with potent antitubercular activity through noncovalent inhibition of decaprenylphosphoryl-β-d-ribose 2′-epimerase (DprE1). Further, this series was optimized to improve its physicochemical properties and pharmacokinetics in mice. Here, we describe the short-listing of a potential clinical candidate, compound 2, that has potent cellular activity, drug-like properties, efficacy in mouse and rat chronic TB infection models, and minimal in vitro safety risks. We also demonstrate that the compounds, including compound 2, have no antagonistic activity with other anti-TB drugs. Moreover, compound 2 shows synergy with PA824 and TMC207 in vitro, and the synergy effect is translated in vivo with TMC207. The series is predicted to have a low clearance in humans, and the predicted human dose for compound 2 is ≤1 g/day. Altogether, our data suggest that a 1,4-azaindole (compound 2) is a promising candidate for the development of a novel anti-TB drug.
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