Diarylthiazole: an antimycobacterial scaffold potentially targeting PrrB-PrrA two-component system was written by Bellale, Eknath;Naik, Maruti;Varun, V. B.;Ambady, Anisha;Narayan, Ashwini;Ravishankar, Sudha;Ramachandran, Vasanthi;Kaur, Parvinder;McLaughlin, Robert;Whiteaker, James;Morayya, Sapna;Guptha, Supreeth;Sharma, Sreevalli;Raichurkar, Anandkumar;Awasthy, Disha;Achar, Vijayshree;Vachaspati, Prakash;Bandodkar, Balachandra;Panda, Manoranjan;Chatterji, Monalisa. And the article was included in Journal of Medicinal Chemistry in 2014.Reference of 214834-18-1 This article mentions the following:
Diarylthiazole (DAT), a hit from diversity screening, was found to have potent antimycobacterial activity against Mycobacterium tuberculosis (Mtb). In a systematic medicinal chem. exploration, the authors demonstrated chem. opportunities to optimize the potency and physicochem. properties. The effort led to more than 10 compounds with submicromolar MICs and desirable physicochem. properties. The potent antimycobacterial activity, in conjunction with low mol. weight, made the series an attractive lead (antibacterial ligand efficiency (ALE) >0.4). The series exhibited excellent bactericidal activity and was active against drug-sensitive and resistant Mtb. Mutational anal. showed that mutations in prrB impart resistance to DAT compounds but not to reference drugs tested. The sensor kinase PrrB belongs to the PrrBA two component system and is potentially the target for DAT. PrrBA is a conserved, essential regulatory mechanism in Mtb and has been shown to have a role in virulence and metabolic adaptation to stress. Hence, DATs provide an opportunity to understand a completely new target system for antimycobacterial drug discovery. In the experiment, the researchers used many compounds, for example, tert-Butyl 4-carbamothioylpiperidine-1-carboxylate (cas: 214834-18-1Reference of 214834-18-1).
tert-Butyl 4-carbamothioylpiperidine-1-carboxylate (cas: 214834-18-1) belongs to pyridine derivatives. Pyridine has a dipole moment and a weaker resonant stabilization than benzene (resonance energy 117 kJ·molâ? in pyridine vs. 150 kJ·molâ? in benzene). Pyridine groups exist in countless molecules, and their applications include catalysis, drug design, molecular recognition, and natural product synthesis.Reference of 214834-18-1