Antitubercular Triazines: Optimization and Intrabacterial Metabolism

Xin Wang,Nisha Mittal,Steve D Paget,Steven Park,Véronique Dartois,Courtney Grady,Daigo Inoyama,Sean Ekins,Riccardo Russo,Srinivasan Kandasamy,Alejandro Davila-Pagan,Richard S Pottorf,Patricia Soteropoulos,Joseph A Bilotta,Thomas P Stratton,Pradeep Kumar,Hsin Pin Ho,Joel S Freundlich,Eric Singleton,Nancy Connell,Thomas Kim,Shao Gang Li ,Ravindra D Jadhav ,Syed M Hussain ,Yong Mo Ahn ,Matthew Zimmerman

doi:10.1016/j.chembiol.2019.10.010

Xin Wang, Nisha Mittal + Show 24 more

Open Access

https://doi.org/10.1016/j.chembiol.2019.10.010

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Abstract

The triazine antitubercular JSF-2019 was of interestdue to its invitro efficacy and the nitro group shared with the clinically relevant delamanid and pretomanid. JSF-2019 undergoes activation requiring F420H2 and one or more nitroreductases in addition to Ddn. An intrabacterial drug metabolism (IBDM) platform was leveraged to demonstrate the system kinetics, evidencing formation of NO⋅ and a des-nitro metabolite. Structure-activity relationship studies focused on improving the solubility and mouse pharmacokinetic profile of JSF-2019 and culminated in JSF-2513, relying on the key introduction of a morpholine. Mechanistic studies with JSF-2019, JSF-2513, and other triazines stressed the significance of achieving potent invitro efficacy via release of intrabacterial NO⋅ along with inhibition of InhA and, more generally, the FAS-II pathway. This study highlights the importance of probing IBDM and its potential to clarify mechanism of action, which in this case is a combination of NO⋅ release and InhA inhibition.

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