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鼠型 I 脂肪酸合酶(FAS)多特异性转移酶的特性及其对聚酮合酶(PKS)工程的影响。

Characterization of the Polyspecific Transferase of Murine Type I Fatty Acid Synthase (FAS) and Implications for Polyketide Synthase (PKS) Engineering.

机构信息

Institute of Organic Chemistry and Chemical Biology, Buchmann Institute for Molecular Life Sciences, Cluster of Excellence for Macromolecular Complexes , Goethe University Frankfurt , Max-von-Laue-Str. 15 , 60438 Frankfurt am Main , Germany.

出版信息

ACS Chem Biol. 2018 Mar 16;13(3):723-732. doi: 10.1021/acschembio.7b00718. Epub 2018 Feb 1.

Abstract

Fatty acid synthases (FASs) and polyketide synthases (PKSs) condense acyl compounds to fatty acids and polyketides, respectively. Both, FASs and PKSs, harbor acyltransferases (ATs), which select substrates for condensation by β-ketoacyl synthases (KSs). Here, we present the structural and functional characterization of the polyspecific malonyl/acetyltransferase (MAT) of murine FAS. We assign kinetic constants for the transacylation of the native substrates, acetyl- and malonyl-CoA, and demonstrate the promiscuity of FAS to accept structurally and chemically diverse CoA-esters. X-ray structural data of the KS-MAT didomain in a malonyl-loaded state suggests a MAT-specific role of an active site arginine in transacylation. Owing to its enzymatic properties and its accessibility as a separate domain, MAT of murine FAS may serve as versatile tool for engineering PKSs to provide custom-tailored access to new polyketides that can be applied in antibiotic and antineoplastic therapy.

摘要

脂肪酸合酶 (FASs) 和聚酮合酶 (PKSs) 分别将酰基化合物缩合为脂肪酸和聚酮。FASs 和 PKSs 都含有酰基转移酶 (ATs),它们通过β-酮酰基合酶 (KSs) 选择缩合的底物。在这里,我们介绍了鼠 FAS 的多特异性丙二酰/乙酰基转移酶 (MAT) 的结构和功能特征。我们为天然底物乙酰-CoA 和丙二酰-CoA 的反酰基转移分配了动力学常数,并证明了 FAS 对结构和化学上不同的 CoA 酯的混杂性。在丙二酰基负载状态下的 KS-MAT 二结构域的 X 射线结构数据表明,一个活性位点精氨酸在反酰基转移中具有 MAT 特异性作用。由于其酶学特性和作为独立结构域的可及性,鼠 FAS 的 MAT 可能成为工程 PKS 的多功能工具,为提供定制的访问新的聚酮提供了可能,这些聚酮可应用于抗生素和抗肿瘤治疗。

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