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- 腺嘌呤-D-甲硫氨酸的甲基化发生在细菌中 1-氨基-2-甲基环丙烷羧酸(诺科罗尼酸)生物合成中的环丙烷化之前。

-Methylation of -adenosyl-L-Methionine Occurs Prior to Cyclopropanation in the Biosynthesis of 1-Amino-2-Methylcyclopropanecarboxylic Acid (Norcoronamic Acid) in a Bacterium.

机构信息

Department of Bioscience, Fukui Prefectural University, 4-1-1 Yoshida-Gun, Fukui 910-1195, Japan.

Department of Chemistry, Tokyo Institute of Technology, 2-12-1 O-okayama, Meguro-ku, Tokyo 152-8551, Japan.

出版信息

Biomolecules. 2020 May 16;10(5):775. doi: 10.3390/biom10050775.

Abstract

Many pharmacologically important peptides are bacterial or fungal in origin and contain nonproteinogenic amino acid (NPA) building blocks. Recently, it was reported that, in bacteria, a cyclopropane-containing NPA 1-aminocyclopropanecarboxylic acid (ACC) is produced from the L-methionine moiety of -adenosyl-L-methionine (SAM) by non-canonical ACC-forming enzymes. On the other hand, it has been suggested that a monomethylated ACC analogue, 2-methyl-ACC (MeACC), is derived from L-valine. Therefore, we have investigated the MeACC biosynthesis by identifying a gene cluster containing bacterial MeACC synthase genes. In this gene cluster, we identified two genes, and , which encode a cobalamin (B12)-dependent radical SAM methyltransferase and a bacterial ACC synthase, respectively, and were found to be involved in the MeACC biosynthesis. In vitro analysis using their recombinant enzymes (rOrf29 and rOrf30) further revealed that the ACC structure of MeACC was derived from the L-methionine moiety of SAM, rather than L-valine. In addition, rOrf29 was found to catalyze the -methylation of the L-methionine moiety of SAM. The resulting methylated derivative of SAM was then converted into MeACC by rOrf30. Thus, we demonstrate that -methylation of SAM occurs prior to cyclopropanation in the biosynthesis of a bacterial MeACC (norcoronamic acid).

摘要

许多具有药理重要性的肽类物质源自细菌或真菌,且含有非蛋白氨基酸(NPA)构建模块。最近,据报道,在细菌中,环丙烷-NPA 1-氨基环丙烷羧酸(ACC)由 -腺苷甲硫氨酸(SAM)的 L-蛋氨酸部分通过非典型的 ACC 形成酶生成。另一方面,有人提出单甲基化的 ACC 类似物 2-甲基-ACC(MeACC)来源于 L-缬氨酸。因此,我们通过鉴定含有细菌 MeACC 合成酶基因的基因簇来研究 MeACC 的生物合成。在这个基因簇中,我们鉴定了两个基因, 和 ,它们分别编码钴胺素(B12)依赖性自由基 SAM 甲基转移酶和细菌 ACC 合成酶,并且被发现参与 MeACC 的生物合成。使用它们的重组酶(rOrf29 和 rOrf30)进行的体外分析进一步表明,MeACC 的 ACC 结构来自 SAM 的 L-蛋氨酸部分,而不是 L-缬氨酸。此外,rOrf29 被发现催化 SAM 的 L-蛋氨酸部分的 -甲基化。然后,rOrf30 将生成的 SAM 甲基化衍生物转化为 MeACC。因此,我们证明了在细菌 MeACC(norcoronamic 酸)生物合成中,SAM 的 -甲基化先于环丙烷化发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8ccc/7277169/070fac7afac3/biomolecules-10-00775-g001.jpg

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