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胞苷衍生物作为伯克霍尔德氏菌的 IspF 抑制剂。

Cytidine derivatives as IspF inhibitors of Burkolderia pseudomallei.

机构信息

Department of Chemistry and Biochemistry, Northern Illinois University, DeKalb, IL, USA.

出版信息

Bioorg Med Chem Lett. 2013 Dec 15;23(24):6860-3. doi: 10.1016/j.bmcl.2013.09.101. Epub 2013 Oct 8.

Abstract

Published biological data suggest that the methyl erythritol phosphate (MEP) pathway, a non-mevalonate isoprenoid biosynthetic pathway, is essential for certain bacteria and other infectious disease organisms. One highly conserved enzyme in the MEP pathway is 2C-methyl-d-erythritol 2,4-cyclodiphosphate synthase (IspF). Fragment-bound complexes of IspF from Burkholderia pseudomallei were used to design and synthesize a series of molecules linking the cytidine moiety to different zinc pocket fragment binders. Testing by surface plasmon resonance (SPR) found one molecule in the series to possess binding affinity equal to that of cytidine diphosphate, despite lacking any metal-coordinating phosphate groups. Close inspection of the SPR data suggest different binding stoichiometries between IspF and test compounds. Crystallographic analysis shows important variations between the binding mode of one synthesized compound and the pose of the bound fragment from which it was designed. The binding modes of these molecules add to our structural knowledge base for IspF and suggest future refinements in this compound series.

摘要

已发表的生物学数据表明,磷酸甲基赤藓醇(MEP)途径是一种非甲羟戊酸异戊烯基生物合成途径,对某些细菌和其他传染病病原体至关重要。MEP 途径中的一种高度保守的酶是 2C-甲基-D-赤藓醇 2,4-环二磷酸合酶(IspF)。利用伯克霍尔德氏菌假单胞菌的 IspF 片段结合复合物,设计并合成了一系列将胞苷部分与不同锌口袋片段结合物连接的分子。表面等离子体共振(SPR)测试发现,该系列中的一种分子具有与胞苷二磷酸相当的结合亲和力,尽管它缺乏任何金属配位的磷酸基团。对 SPR 数据的仔细检查表明,IspF 与测试化合物之间的结合化学计量存在差异。晶体学分析表明,一种合成化合物的结合模式与设计它的结合片段的构象之间存在重要差异。这些分子的结合模式增加了我们对 IspF 的结构知识库,并为该化合物系列的未来改进提供了依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/98d8/3874807/0a2e249bd9e7/nihms531500f1.jpg

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Cytidine derivatives as IspF inhibitors of Burkolderia pseudomallei.胞苷衍生物作为伯克霍尔德氏菌的 IspF 抑制剂。
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