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HIV-1蛋白酶的二聚化抑制剂

Dimerization inhibitors of HIV-1 protease.

作者信息

Boggetto Nicole, Reboud-Ravaux Michèle

机构信息

Département de Biologie Cellulaire, Institut Jacques Monod, UMR 7592, CNRS-Université Paris 6, France.

出版信息

Biol Chem. 2002 Sep;383(9):1321-4. doi: 10.1515/BC.2002.150.

Abstract

By targeting the highly conserved antiparallel beta-sheet formed by the interdigitation of the N- and C-terminal strands of each monomer, dimerization inhibitors of HIV-1 protease may be useful to overcome the drug resistance observed with current active-site directed antiproteases. Sequestration of the monomer by the inhibitor (or disruption of the dimer interface) prevents the correct assembly of the inactive monomers to active enzyme. Strategies for the design of drugs targeting the dimer interface are described. Various dimerization inhibitors are reported including N- and C-terminal mimetics, lipopeptides and cross-linked interface peptides.

摘要

通过靶向由每个单体的N端和C端链相互交叉形成的高度保守的反平行β-折叠,HIV-1蛋白酶的二聚化抑制剂可能有助于克服目前针对活性位点的抗蛋白酶所观察到的耐药性。抑制剂对单体的隔离(或二聚体界面的破坏)可防止无活性单体正确组装成活性酶。本文描述了靶向二聚体界面的药物设计策略。报道了各种二聚化抑制剂,包括N端和C端模拟物、脂肽和交联界面肽。

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