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LIGANDS THAT TARGET HCV-E2 BINDING SITES ON CD81 AND THERAPEUTIC METHODS USING THEM

机译:将HCV-E2结合位点靶向CD81的配体及其治疗方法

摘要

Ligands that target the HCV-E2 binding site and methods of making and using them. A series of ligand binding sites on the large extracellular loop of the open conformation of CD81 have been identified. Several important sites were located in regions identified by mutational studies to be the site of E2 binding. Ligands that recognize these sites were identified. Linking together two or three ligands that bind with low or moderate affinities to different structurally unique sites on a target protein were used to generate small molecule ligand conjugates that exhibit very high affinities to their CD81 targets. Hybrid ligand molecules were also designed using fragment-based drug design methods to generate analogs of the ligands that bind more tightly to the protein than the parent compounds. Identification and design of groups of compounds that bind to CD81 for use as therapeutics for treating patients infected by Hepatitis C virus and other viruses that interact with CD81. By binding to CD81, these molecules can block 1) HCV and other viral entry into cells (infection), 2) inflammatory responses caused by HCV and other viral infections, and 3) the induction of HCV associated cancers.
机译:靶向HCV-E2结合位点的配体及其制备和使用方法。已经鉴定出CD81开放构象的大细胞外环上的一系列配体结合位点。几个重要的位点位于通过突变研究确定为E2结合位点的区域。确定了识别这些位点的配体。将以低或中等亲和力结合至靶蛋白上不同结构独特位点的两个或三个配体连接在一起,以产生对CD81靶表现出非常高亲和力的小分子配体缀合物。还使用基于片段的药物设计方法设计了杂合配体分子,以生成与母体化合物相比与蛋白质结合更紧密的配体类似物。鉴定和设计与CD81结合的化合物组,用作治疗被丙型肝炎病毒和其他与CD81相互作用的病毒感染的患者的治疗剂。通过与CD81结合,这些分子可以阻断1)HCV和其他病毒进入细胞(感染),2)HCV和其他病毒感染引起的炎症反应,以及3)HCV相关癌症的诱导。

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