Synthesis and evaluation of pyridine-derived bedaquiline analogues containing modifications at the A-ring subunit

Lisa Barbaro; Gayathri Nagalingam; James A Triccas; Lendl Tan; Nicholas P West; Jonathan B Baell; Daniel L Priebbenow

doi:10.1039/d1md00063b

Synthesis and evaluation of pyridine-derived bedaquiline analogues containing modifications at the A-ring subunit

RSC Med Chem. 2021 May 7;12(6):943-959. doi: 10.1039/d1md00063b. eCollection 2021 Jun 23.

Authors

Lisa Barbaro¹, Gayathri Nagalingam², James A Triccas², Lendl Tan^{3

4}, Nicholas P West^{3

4}, Jonathan B Baell¹, Daniel L Priebbenow⁵

Affiliations

¹ Monash Institute of Pharmaceutical Sciences, Monash University 381 Royal Parade Parkville Victoria 3052 Australia [email protected].
² School of Medical Sciences and Marie Bashir Institute, The University of Sydney Sydney NSW 2006 Australia.
³ School of Chemistry and Molecular Bioscience, The University of Queensland St Lucia Queensland 4072 Australia.
⁴ Australian Infectious Diseases Research Centre St. Lucia Queensland 4067 Australia.
⁵ School of Chemistry, The University of Melbourne Parkville Victoria 3010 Australia [email protected].

Abstract

Despite promising efficacy, the clinical use of the anti-tubercular therapeutic bedaquiline has been restricted due to safety concerns. To date, limited SAR studies have focused on the quinoline ring (A-ring), and as such, we set out to explore modifications within this region in an attempt to discover new bedaquiline variants with an improved safety profile. We herein report the development of unique synthetic strategies that facilitated access to novel bedaquiline analogues leading to the discovery that anti-tubercular activity could be retained following replacement of the quinoline motif with pyridine heterocycles. This discovery is anticipated to open up multiple new avenues for exploration in the design of improved anti-tubercular therapeutics.