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Crystal structure of bifunctional transglycosylase PBP1b from E. coli and inhibitors thereof

机译：来自E的双功能转糖基转移酶PBP1b的晶体结构。大肠杆菌及其抑制剂

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摘要

The crystal structure at 2.16 Å resolution of the full-length bacterial bifunctional transglycosylase penicillin-binding protein 1b (PBP1b) from Escherichia coli, in complex with its inhibitor moenomycin, is provided. The atomic coordinates of the complex as well as the moenomycin binding site are provided. Three dimensional structures of amino acid residues involved in moenomycin binding and transglycosylation activity are identified. Binding site for peptidoglycan synthesis inhibitors comprising inhibitor-binding site comprises amino acid residues from at least one of transglycosylase (TG), UvrB domain 2 homolog (UB2H) and transmembrane (TM) domains of PBP1b are identified at an atomic level of resolution. Methods for rational drug design based on the atomic coordinates are provided. Methods for screening for antibiotics based on anisotropic binding assay and transglycosylase inhibitor assays are provided. Novel antibiotics based on the screening assays of the invention are disclosed.

机译：提供了大肠杆菌的全长细菌双功能转糖基转移酶青霉素结合蛋白1b（PBP1b）及其抑制剂moenomycin的晶体结构，分辨率为2.16Å。提供了配合物的原子坐标以及新霉素结合位点。确定了与莫诺霉素结合和转糖基化活性有关的氨基酸残基的三维结构。包含抑制剂结合位点的肽聚糖合成抑制剂的结合位点包含来自PBP1b的转糖基化酶（TG），UvrB结构域2同源物（UB2H）和跨膜（TM）结构域中至少一个的氨基酸残基，这些原子残基是通过分辨率的原子级鉴定的。提供了基于原子坐标的合理药物设计方法。提供了基于各向异性结合测定和转糖基酶抑制剂测定的抗生素筛选方法。公开了基于本发明的筛选测定法的新型抗生素。 展开▼

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公开/公告号US9890111B2

专利类型

公开/公告日2018-02-13

原文格式PDF

申请/专利权人 ACADEMIA SINICA;
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申请/专利号US201514960025

发明设计人 CHE ALEX MA;CHI-HUEY WONG;WEI-CHIEH CHENG;TING-JEN RACHEL CHENG;
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申请日2015-12-04

分类号C07C235/64;C12Q1/18;C12Q1/48;C07C235/84;

国家 US

入库时间 2022-08-21 12:58:18

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