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在两种海洋细菌中鉴定出跨 AT 聚酮化合物簇,揭示了不同共生因子之间隐藏的相似性。

Identification of trans-AT polyketide clusters in two marine bacteria reveals cryptic similarities between distinct symbiosis factors.

机构信息

Department of Microbial and Plant Biotechnology, Centro de Investigaciones Biológicas Margarita Salas, Agencia Estatal Consejo Superior de Investigaciones Científicas (CSIC), Madrid, Spain.

Research and Development Department, PharmaMar S.A., Madrid, Spain.

出版信息

Environ Microbiol. 2021 May;23(5):2509-2521. doi: 10.1111/1462-2920.15470. Epub 2021 Apr 2.

DOI:10.1111/1462-2920.15470
PMID:33734547
Abstract

Glutarimide-containing polyketides are known as potent antitumoral and antimetastatic agents. The associated gene clusters have only been identified in a few Streptomyces producers and Burkholderia gladioli symbiont. The new glutarimide-family polyketides, denominated sesbanimides D, E and F along with the previously known sesbanimide A and C, were isolated from two marine alphaproteobacteria Stappia indica PHM037 and Labrenzia aggregata PHM038. Structures of the isolated compounds were elucidated based on 1D and 2D homo and heteronuclear NMR analyses and ESI-MS spectrometry. All compounds exhibited strong antitumor activity in lung, breast and colorectal cancer cell lines. Subsequent whole genome sequencing and genome mining revealed the presence of the trans-AT PKS gene cluster responsible for the sesbanimide biosynthesis, described as sbn cluster. Strikingly, the modular architecture of downstream mixed type PKS/NRPS, SbnQ, revealed high similarity to PedH in pederin and Lab13 in labrenzin gene clusters, although those clusters are responsible for the production of structurally completely different molecules. The unexpected presence of SbnQ homologues in unrelated polyketide gene clusters across phylogenetically distant bacteria, raises intriguing questions about the evolutionary relationship between glutarimide-like and pederin-like pathways, as well as the functionality of their synthetic products.

摘要

含戊二酰亚胺的聚酮类化合物是具有强效抗肿瘤和抗转移作用的物质。相关基因簇仅在少数链霉菌产生菌和柄杆菌属(Burkholderia)gladioli 共生菌中被发现。新的戊二酰亚胺家族聚酮类化合物,即 sesbanimides D、E 和 F 以及先前已知的 sesbanimide A 和 C,是从两种海洋 α-变形菌 Stappia indica PHM037 和 Labrenzia aggregata PHM038 中分离得到的。根据 1D 和 2D 同核和异核 NMR 分析和 ESI-MS 光谱学,确定了分离化合物的结构。所有化合物在肺癌、乳腺癌和结直肠癌细胞系中均表现出强烈的抗肿瘤活性。随后的全基因组测序和基因组挖掘揭示了负责 sesbanimide 生物合成的 trans-AT PKS 基因簇的存在,称为 sbn 簇。引人注目的是,下游混合类型 PKS/NRPS、SbnQ 的模块化结构与 pederin 中的 PedH 和 labrenzin 基因簇中的 Lab13 高度相似,尽管这些簇负责产生结构完全不同的分子。在系统发育上相距甚远的细菌中, unrelated polyketide 基因簇中存在 SbnQ 同源物,这引发了关于戊二酰亚胺样和 pederin 样途径之间的进化关系以及它们的合成产物的功能的有趣问题。

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