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天然产物甲基转移酶的结构、机制和分子进化。

Architectures, mechanisms and molecular evolution of natural product methyltransferases.

机构信息

Howard Hughes Medical Institute, Jack H. Skirball Center for Chemical Biology and Proteomics, Salk Institute for Biological Studies, La Jolla, CA 92037, USA.

出版信息

Nat Prod Rep. 2012 Oct;29(10):1238-50. doi: 10.1039/c2np20029e. Epub 2012 Aug 1.

Abstract

The addition of a methyl moiety to a small chemical is a common transformation in the biosynthesis of natural products across all three domains of life. These methylation reactions are most often catalysed by S-adenosyl-L-methionine (SAM)-dependent methyltransferases (MTs). MTs are categorized based on the electron-rich, methyl accepting atom, usually O, N, C, or S. SAM-dependent natural product MTs (NPMTs) are responsible for the modification of a wide array of structurally distinct substrates, including signalling and host defense compounds, pigments, prosthetic groups, cofactors, cell membrane and cell wall components, and xenobiotics. Most notably, methylation modulates the bioavailability, bioactivity, and reactivity of acceptor molecules, and thus exerts a central role on the functional output of many metabolic pathways. Our current understanding of the structural enzymology of NPMTs groups these phylogenetically diverse enzymes into two MT-superfamily fold classes (class I and class III). Structural biology has also shed light on the catalytic mechanisms and molecular bases for substrate specificity for over fifty NPMTs. These biophysical-based approaches have contributed to our understanding of NPMT evolution, demonstrating how a widespread protein fold evolved to accommodate chemically diverse methyl acceptors and to catalyse disparate mechanisms suited to the physiochemical properties of the target substrates. This evolutionary diversity suggests that NPMTs may serve as starting points for generating new biocatalysts.

摘要

在所有生命的三个领域中,在小化学物质上添加一个甲基是天然产物生物合成中的常见转化。这些甲基化反应通常由 S-腺苷-L-甲硫氨酸(SAM)依赖性甲基转移酶(MTs)催化。MT 基于电子供体、甲基受体原子进行分类,通常为 O、N、C 或 S。SAM 依赖性天然产物 MT(NPMT)负责修饰广泛的结构不同的底物,包括信号和宿主防御化合物、色素、辅基、辅酶、细胞膜和细胞壁成分以及外来物质。值得注意的是,甲基化调节了受体分子的生物利用度、生物活性和反应性,因此对许多代谢途径的功能输出起着核心作用。我们目前对 NPMT 的结构酶学的理解将这些系统发育多样化的酶分为两类 MT 超家族折叠类(I 类和 III 类)。结构生物学还揭示了五十多种 NPMT 的催化机制和底物特异性的分子基础。这些基于生物物理的方法有助于我们理解 NPMT 的进化,表明广泛的蛋白质折叠如何进化以适应化学性质不同的甲基受体,并催化适合于目标底物物理化学性质的不同机制。这种进化多样性表明,NPMT 可能成为产生新生物催化剂的起点。

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