| Literature DB >> 24900867 |
Chaitanya Kumar Kedari1, Nilanjana Roy Choudhury2, Sreevalli Sharma2, Parvinder Kaur2, Supreeth Guptha2, Manoranjan Panda2, Kakoli Mukerjee1, Vasanthi Ramachandran2, Balachandra Bandodkar1, Sreekanth Ramachandran2, Subramanyam J Tantry2.
Abstract
A whole cell based screening effort on a focused library from corporate collection resulted in the identification of biarylmethoxy nicotinamides as novel inhibitors of M. tuberculosis (Mtu) H37Rv. The series exhibited tangible structure-activity relationships, and during hit to lead exploration, a cellular potency of 100 nM was achieved, which is an improvement of >200-fold from the starting point. The series is very specific to Mtu and noncytotoxic up to 250 μM as measured in the mammalian cell line THP-1 based cytotoxicity assay. This compound class retains its potency on several drug sensitive and single drug resistant clinical isolates, which indicate that the compounds could be acting through a novel mode of action.Entities:
Keywords: MMIC; anti-TB; biarylmethoxy nicotinamides; clinical isolates
Year: 2014 PMID: 24900867 PMCID: PMC4027638 DOI: 10.1021/ml4004815
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345