首页> 外文期刊>Journal of Molecular Biology >Structure of the human fatty acid synthase KS-MAT didomain as a framework for inhibitor design.
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Structure of the human fatty acid synthase KS-MAT didomain as a framework for inhibitor design.

机译:人脂肪酸合酶KS-MAT双结构域的结构作为抑制剂设计的框架。

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摘要

The human fatty acid synthase (FAS) is a key enzyme in the metabolism of fatty acids and a target for antineoplastic and antiobesity drug development. Due to its size and flexibility, structural studies of mammalian FAS have been limited to individual domains or intermediate-resolution studies of the complete porcine FAS. We describe the high-resolution crystal structure of a large part of human FAS that encompasses the tandem domain of beta-ketoacyl synthase (KS) connected by a linker domain to the malonyltransferase (MAT) domain. Hinge regions that allow for substantial flexibility of the subdomains are defined. The KS domain forms the canonical dimer, and its substrate-binding site geometry differs markedly from that of bacterial homologues but is similar to that of the porcine orthologue. The didomain structure reveals a possible way to generate a small and compact KS domain by omitting a large part of the linker and MAT domains, which could greatly aid in rapid screening of KS inhibitors. In the crystal, the MAT domain exhibits two closed conformations that differ significantly by rigid-body plasticity. This flexibility may be important for catalysis and extends the conformational space previously known for type I FAS and 6-deoxyerythronolide B synthase.
机译:人脂肪酸合酶(FAS)是脂肪酸代谢中的关键酶,是抗肿瘤药和抗肥胖药开发的目标。由于其大小和灵活性,哺乳动物FAS的结构研究仅限于单个域或完整猪FAS的中等分辨率研究。我们描述了人类FAS的很大一部分的高分辨率晶体结构,该结构包含β-酮酰基合酶(KS)的串联结构域,该结构域通过接头结构域连接至丙二酰转移酶(MAT)结构域。定义了允许子域具有相当大灵活性的铰链区域。 KS结构域形成规范的二聚体,其底物结合位点的几何形状与细菌同源物明显不同,但与猪直向同源物相似。双结构域结构揭示了通过省略大部分连接子和MAT结构域来生成小而紧凑的KS结构域的可能方法,这可以极大地帮助快速筛选KS抑制剂。在晶体中,MAT域显示出两个闭合构象,这些构象在刚体可塑性方面明显不同。这种灵活性对于催化可能很重要,并且可以扩展先前已知的I型FAS和6-脱氧赤藓醇B合酶的构象空间。

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