| Literature DB >> 19874035 |
Pavlína Rezácová1, Jana Pokorná, Jirí Brynda, Milan Kozísek, Petr Cígler, Martin Lepsík, Jindrich Fanfrlík, Jan Rezác, Klára Grantz Sasková, Irena Sieglová, Jaromír Plesek, Václav Sícha, Bohumír Grüner, Heike Oberwinkler, Juraj Sedlácek', Hans-Georg Kräusslich, Pavel Hobza, Vladimír Král, Jan Konvalinka.
Abstract
HIV protease (HIV PR) is a primary target for anti-HIV drug design. We have previously identified and characterized substituted metallacarboranes as a new class of HIV protease inhibitors. In a structure-guided drug design effort, we connected the two cobalt bis(dicarbollide) clusters with a linker to substituted ammonium group and obtained a set of compounds based on a lead formula [H(2)N-(8-(C(2)H(4)O)(2)-1,2-C(2)B(9)H(10))(1',2'-C(2)B(9)H(11))-3,3'-Co)(2)]Na. We explored inhibition properties of these compounds with various substitutions, determined the HIV PR:inhibitor crystal structure, and computationally explored the conformational space of the linker. Our results prove the capacity of linker-substituted dual-cage cobalt bis(dicarbollides) as lead compounds for design of more potent inhibitors of HIV PR.Entities:
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Year: 2009 PMID: 19874035 DOI: 10.1021/jm9011388
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446