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X-Ray Structure of Human Fpps and Use For Selecting Fpps Binding Compounds

机译:人类Fpps的X射线结构及其在选择Fpps结合化合物中的用途

摘要

The present invention relates to crystalline human farnesyl diphosphate synthase (FPPS), to the three-dimensional structure of free FPPS as well as the three-dimensional structures of FPPS in complex with substrates such as IPP (isopentenyl diphosphate) and/or with inhibitors such as Zometa® or Aredia®. Further, methods for preparing crystals of human FPPS are described. According to the invention the crystals can be used to determine the structures of FPPS homologs mutants, complexes with ligands, FPPS crystal forms and similar molecules of unknown structure. The invention further relates to the use of FPPS crystals to select new FPPS ligands, e.g. by X-ray screening and to design and/or identify inhibitors against FPPS. Furthermore, the invention relates to NMR methods for selecting and/or identifying new low molecular weight binders to FPPS, which represent new therapeutic agents.
机译:本发明涉及结晶人法呢基二磷酸合酶(FPPS),游离FPPS的三维结构以及与底物如IPP(异戊烯基二磷酸)复合和/或与抑制剂结合的FPPS的三维结构。作为Zometa®或Aredia®。此外,描述了制备人FPPS晶体的方法。根据本发明,晶体可以用于确定FPPS同源突变体,与配体的复合物,FPPS晶体形式和未知结构的相似分子的结构。本发明还涉及FPPS晶体用于选择新的FPPS配体的用途,例如,FPPS晶体。通过X射线筛查以及设计和/或鉴定针对FPPS的抑制剂。此外,本发明涉及用于选择和/或鉴定代表新型治疗剂的FPPS的新的低分子量粘合剂的NMR方法。

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