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Nitroarenes as Antitubercular Agents: Stereoelectronic Modulation to Mitigate Mutagenicity
Authors:Dr. Sudhir Landge  Dr. Vasanthi Ramachandran  Dr. Anupriya Kumar  Dr. João Neres  Kannan Murugan  Dr. Claire Sadler  Dr. Mick D. Fellows  Vaishali Humnabadkar  Dr. Prakash Vachaspati  Dr. Anandkumar Raichurkar  Sreevalli Sharma  Sudha Ravishankar  Supreeth Guptha  Dr. Vasan K. Sambandamurthy  Dr. Tanjore S. Balganesh  Dr. Bheemarao G. Ugarkar  Dr. V. Balasubramanian  Dr. Balachandra S. Bandodkar  Dr. Manoranjan Panda
Affiliation:1. iMED Infection, AstraZeneca India Pvt. Ltd., Bangalore, India;2. Global Health Institute, école Polytechnique Fédérale de Lausanne (EPFL), Lausanne, Switzerland;3. iMED Safety Assessment, AstraZeneca, Macclesfield, UK;4. Biocon Bristol-Myers Squibb Research Center, Biocon Park, Bangalore, India
Abstract:Nitroarenes are less preferred in drug discovery due to their potential to be mutagenic. However, several nitroarenes were shown to be promising antitubercular agents with specific modes of action, namely, nitroimidazoles and benzothiazinones. The nitro group in these compounds is activated through different mechanisms, both enzymatic and non‐enzymatic, in mycobacteria prior to binding to the target of interest. From a whole‐cell screening program, we identified a novel lead nitrobenzothiazole (BT) series that acts by inhibition of decaprenylphosphoryl‐β‐d ‐ribose 2′‐epimerase (DprE1) of Mycobacterium tuberculosis (Mtb). The lead was found to be mutagenic to start with. Our efforts to mitigate mutagenicity resulted in the identification of 6‐methyl‐7‐nitro‐5‐(trifluoromethyl)‐1,3‐benzothiazoles (cBTs), a novel class of antitubercular agents that are non‐mutagenic and exhibit an improved safety profile. The methyl group ortho to the nitro group decreases the electron affinity of the series, and is hence responsible for the non‐mutagenic nature of these compounds. Additionally, the co‐crystal structure of cBT in complex with Mtb DprE1 established the mode of binding. This investigation led to a new non‐mutagenic antitubercular agent and demonstrates that the mutagenic nature of nitroarenes can be solved by modulation of stereoelectronic properties.
Keywords:ab   initio calculations  antitubercular agents  density functional theory  electron affinity  mutagenicity  nitroarenes
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