| Literature DB >> 33316407 |
Shuichi Sugiyama1, Toshiyuki Akiyama2, Yoshiyuki Taoda2, Tsutomu Iwaki2, Eriko Matsuoka2, Erika Akihisa2, Takahiro Seki2, Tomokazu Yoshinaga2, Takashi Kawasuji2.
Abstract
We have discovered HIV-1 novel integrase-LEDGF/p75 allosteric inhibitors (INLAIs) based on a pyridine scaffold forming an intramolecular hydrogen bond. Scaffolds containing a pyridine moiety have been studied extensively and we have already reported that substituents extending from the C1 position contributed to the antiviral potency. In this study, we designed a new pyridine scaffold 2 with a substituent at the C1 position. Interestingly, during attempts at optimization, we found that the direction of the C1 substituents with an intramolecular hydrogen bond contributed to the antiviral potency. Compound 34f exhibited better antiviral potency against WT and the T174I mutant (EC50 (WT) = 6.6 nM, EC50 (T174I) = 270 nM) than BI 224436 (EC50 (WT) = 22 nM, EC50 (T174I) > 5000 nM).Entities:
Keywords: HIV integrase; INLAIs (integrase-LEDGF/p75 allosteric inhibitors); LEDGF (lens epithelium-derived growth factor)
Year: 2020 PMID: 33316407 DOI: 10.1016/j.bmcl.2020.127742
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823