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Virtual Screening Identifies Novel and Potent Inhibitors of Mycobacterium tuberculosis PknB with Antibacterial Activity.

Paptawan ThongdeeChayanin HanwarinrojBongkochawan PakamwongPharit KamsriAuradee PunkvangJiraporn LeanpolchareanchaiSombat KetratPatchreenart SaparpakornSupa HannongbuaKanchiyaphat AriyachaokunKhomson SuttisintongSanya SureramPrasat KittakoopPoonpilas HongmaneePitak SantanirandGalina V MukamolovaRosemary A BloodYuiko TakebayashiJames SpencerAdrian J MulhollandPornpan Pungpo
Published in: Journal of chemical information and modeling (2022)
Mycobacterium tuberculosis protein kinase B (PknB) is essential to mycobacterial growth and has received considerable attention as an attractive target for novel anti-tuberculosis drug development. Here, virtual screening, validated by biological assays, was applied to select candidate inhibitors of M. tuberculosis PknB from the Specs compound library (www.specs.net). Fifteen compounds were identified as hits and selected for in vitro biological assays, of which three indoles ( 2 , AE-848/42799159; 4 , AH-262/34335013; 10 , AP-124/40904362) inhibited growth of M. tuberculosis H37Rv with minimal inhibitory concentrations of 6.2, 12.5, and 6.2 μg/mL, respectively. Two compounds, 2 and 10 , inhibited M. tuberculosis PknB activity in vitro , with IC 50 values of 14.4 and 12.1 μM, respectively, suggesting this to be the likely basis of their anti-tubercular activity. In contrast, compound 4 displayed anti-tuberculosis activity against M. tuberculosis H37Rv but showed no inhibition of PknB activity (IC 50 > 128 μM). We hypothesize that hydrolysis of its ethyl ester to a carboxylate moiety generates an active species that inhibits other M. tuberculosis enzymes. Molecular dynamics simulations of modeled complexes of compounds 2 , 4 , and 10 bound to M. tuberculosis PknB indicated that compound 4 has a lower affinity for M. tuberculosis PknB than compounds 2 and 10 , as evidenced by higher calculated binding free energies, consistent with experiment. Compounds 2 and 10 therefore represent candidate inhibitors of M. tuberculosis PknB that provide attractive starting templates for optimization as anti-tubercular agents.
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