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酰胺合成酶的发现、鉴定及工程改造。

Discovery, characterization and engineering of ligases for amide synthesis.

机构信息

Department of Chemistry, Manchester Institute of Biotechnology, The University of Manchester, Manchester, UK.

School of Food Science and Engineering, South China University of Technology, Guangzhou, China.

出版信息

Nature. 2021 May;593(7859):391-398. doi: 10.1038/s41586-021-03447-w. Epub 2021 May 19.

Abstract

Coronatine and related bacterial phytotoxins are mimics of the hormone jasmonyl-L-isoleucine (JA-Ile), which mediates physiologically important plant signalling pathways. Coronatine-like phytotoxins disrupt these essential pathways and have potential in the development of safer, more selective herbicides. Although the biosynthesis of coronatine has been investigated previously, the nature of the enzyme that catalyses the crucial coupling of coronafacic acid to amino acids remains unknown. Here we characterize a family of enzymes, coronafacic acid ligases (CfaLs), and resolve their structures. We found that CfaL can also produce JA-Ile, despite low similarity with the Jar1 enzyme that is responsible for ligation of JA and L-Ile in plants. This suggests that Jar1 and CfaL evolved independently to catalyse similar reactions-Jar1 producing a compound essential for plant development, and the bacterial ligases producing analogues toxic to plants. We further demonstrate how CfaL enzymes can be used to synthesize a diverse array of amides, obviating the need for protecting groups. Highly selective kinetic resolutions of racemic donor or acceptor substrates were achieved, affording homochiral products. We also used structure-guided mutagenesis to engineer improved CfaL variants. Together, these results show that CfaLs can deliver a wide range of amides for agrochemical, pharmaceutical and other applications.

摘要

冠菌素和相关的细菌植物毒素是激素茉莉酸-L-异亮氨酸 (JA-Ile) 的模拟物,它介导着生理上重要的植物信号通路。冠菌素类植物毒素会破坏这些必要的通路,并且有可能开发出更安全、更具选择性的除草剂。尽管以前已经研究过冠菌素的生物合成,但催化冠芳酸与氨基酸关键偶联的酶的性质仍然未知。在这里,我们描述了一类酶,即冠芳酸连接酶 (CfaL),并解析了它们的结构。我们发现 CfaL 也可以产生 JA-Ile,尽管与负责植物中 JA 和 L-异亮氨酸连接的 Jar1 酶相似度较低。这表明 Jar1 和 CfaL 是独立进化来催化类似反应的——Jar1 产生一种对植物发育至关重要的化合物,而细菌连接酶则产生对植物有毒的类似物。我们进一步展示了 CfaL 酶如何用于合成各种酰胺,从而避免了保护基团的需要。通过高选择性动力学拆分外消旋供体或受体底物,获得了等手性产物。我们还使用结构指导的突变来设计改良的 CfaL 变体。总之,这些结果表明 CfaLs 可以为农业化学、制药和其他应用提供广泛的酰胺。

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