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对来自一种植物相关细菌的细胞毒性聚酮类生物碱贾努他汀A中杂环生物合成的见解。

Insights into Heterocycle Biosynthesis in the Cytotoxic Polyketide Alkaloid Janustatin A from a Plant-Associated Bacterium.

作者信息

Leopold-Messer Stefan, Chawengrum Pornsuda, Piel Jörn

机构信息

Institute of Microbiology, Eidgenössische Technische Hochschule (ETH) Zurich, Vladimir-Prelog-Weg 4, 8093 Zurich, Switzerland.

Chemical Biology Program, Chulabhorn Graduate Institute, Chulabhorn Royal Academy, Kamphaeng Phet 6 Road, Laksi, Bangkok 10210, Thailand.

出版信息

Biochemistry. 2025 Jan 21;64(2):357-363. doi: 10.1021/acs.biochem.4c00542. Epub 2025 Jan 9.

Abstract

Janustatin A is a potently cytotoxic polyketide alkaloid produced at trace amounts by the marine bacterial plant symbiont . Its biosynthetic terminus features an unusual pyridine-containing bicyclic system of unclear origin, in which polyketide and amino acid extension units appear reversed compared to the order of enzymatic modules in the polyketide synthase (PKS)-nonribosomal peptide synthetase (NRPS) assembly line. To elucidate unknown steps in heterocycle formation, we first established robust genome engineering tools in . . A combination of gene deletion, complementation, production improvement, and NMR experiments then demonstrated that two desaturase homologues, JanA and JanB, are involved in hydroxylation and pyridine formation by desaturation, respectively. Structure-activity relationship studies showed that these modifications substantially increase the cytotoxicity and that the fully functionalized heterocyclic system is crucial for sub-nanomolar cytotoxicity. Isolation of the early post-PKS intermediate janustatin D with an already reversed heterocycle topology supports a noncanonical rearrangement process occurring on the PKS-NRPS assembly line.

摘要

贾努他汀A是一种由海洋细菌植物共生体微量产生的具有强细胞毒性的聚酮生物碱。其生物合成末端具有一个来源不明的不寻常的含吡啶双环系统,其中聚酮和氨基酸延伸单元的排列顺序与聚酮合酶(PKS)-非核糖体肽合成酶(NRPS)装配线上酶模块的顺序相反。为了阐明杂环形成中的未知步骤,我们首先在……中建立了强大的基因组工程工具。基因缺失、互补、产量提高和核磁共振实验相结合,证明了两个去饱和酶同源物JanA和JanB分别参与了羟基化和通过去饱和形成吡啶的过程。构效关系研究表明,这些修饰显著提高了细胞毒性,并且完全功能化的杂环系统对于亚纳摩尔级的细胞毒性至关重要。分离出具有已反转杂环拓扑结构的PKS后早期中间体贾努他汀D,支持了在PKS-NRPS装配线上发生的非经典重排过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38df/11755721/e06614c7f2f1/bi4c00542_0001.jpg

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