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研究抗囊素生物合成揭示枯草芽孢杆菌中四酶途径合成四氢酪氨酸。

Investigation of anticapsin biosynthesis reveals a four-enzyme pathway to tetrahydrotyrosine in Bacillus subtilis.

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

Biochemistry. 2010 Feb 9;49(5):912-23. doi: 10.1021/bi9021186.

DOI:10.1021/bi9021186
PMID:20052993
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2819075/
Abstract

Bacillus subtilis produces the antibiotic anticapsin as an L-Ala-L-anticapsin dipeptide precursor known as bacilysin, whose synthesis is encoded by the bacA-D genes and the adjacent ywfGH genes. To evaluate the biosynthesis of the epoxycyclohexanone amino acid anticapsin from the primary metabolite prephenate, we have overproduced, purified, and characterized the activity of the BacA, BacB, YwfH, and YwfG proteins. BacA is an unusual prephenate decarboxylase that avoids the typical aromatization of the cyclohexadienol ring by protonating C(8) to produce an isomerized structure. BacB then catalyzes an allylic isomerization, generating a conjugated dienone with a 295 nm chromophore. Both the BacA and BacB products are regioisomers of H(2)HPP (dihydro-4-hydroxyphenylpyruvate). The BacB product is then a substrate for the short chain reductase YwfH which catalyzes the conjugate addition of hydride at the C(4) olefinic terminus using NADH to yield the cyclohexenol-containing tetrahydro-4-hydroxyphenylpyruvate H(4)HPP. In turn, this keto acid is a substrate for YwfG, which promotes transamination (with L-Phe as amino donor), to form tetrahydrotyrosine (H(4)Tyr). Thus BacA, BacB, YwfH, and YwfG act in sequence in a four enzyme pathway to make H(4)Tyr, which has not previously been identified in B. subtilis but is a recognized building block in cyanobacterial nonribosomal peptides such as micropeptins and aeruginopeptins.

摘要

枯草芽孢杆菌产生抗生素 anticapsin 作为一种 L-Ala-L-anticapsin 二肽前体,称为 bacilysin,其合成由 bacA-D 基因和相邻的 ywfGH 基因编码。为了评估环氧环己烷氨基酸 anticapsin 从初级代谢物预苯酸盐的生物合成,我们已经过表达、纯化和表征了 BacA、BacB、YwfH 和 YwfG 蛋白的活性。BacA 是一种不寻常的预苯酸盐脱羧酶,通过质子化 C(8)来避免环己二烯醇环的典型芳构化,从而产生异构化结构。BacB 然后催化烯丙基异构化,生成具有 295nm 发色团的共轭二烯酮。BacA 和 BacB 的产物都是 H(2)HPP(二氢-4-羟基苯丙酮酸)的区域异构体。BacB 的产物是短链还原酶 YwfH 的底物,该酶使用 NADH 催化 C(4)烯丙基末端的共轭加成,生成含有环己烯醇的四氢-4-羟基苯丙酮酸 H(4)HPP。反过来,这种酮酸是 YwfG 的底物,它促进转氨基作用(以 L-Phe 作为氨基供体),形成四氢酪氨酸(H(4)Tyr)。因此,BacA、BacB、YwfH 和 YwfG 依次在一个四酶途径中作用,生成 H(4)Tyr,这在枯草芽孢杆菌中以前没有被鉴定过,但在蓝细菌非核糖体肽中是一种公认的结构单元,如 micropeptins 和 aeruginopeptins。

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