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坎伯里丁 A 和 B:来自弓背蚁肠道细菌的抗转移和抗炎聚酮生物碱。

Camporidines A and B: Antimetastatic and Anti-inflammatory Polyketide Alkaloids from a Gut Bacterium of Camponotus kiusiuensis.

机构信息

Natural Products Research Institute, College of Pharmacy , Seoul National University , Seoul 08826 , Republic of Korea.

Department of Chemistry and Nanoscience , Ewha Womans University , Seoul 03760 , Republic of Korea.

出版信息

J Nat Prod. 2019 Apr 26;82(4):903-910. doi: 10.1021/acs.jnatprod.8b01000. Epub 2019 Mar 26.

DOI:10.1021/acs.jnatprod.8b01000
PMID:30912943
Abstract

Chemical studies of gut bacteria of the carpenter ant Camponotus kiusiuensis led to the discovery of two new alkaloids, camporidines A and B (1 and 2), from Streptomyces sp. STA1. The structures of 1 and 2 were established as new polyketide alkaloids bearing a piperidine-cyclopentene-epoxide 6/5/3 tricyclic system based on NMR spectroscopic and mass spectrometric analysis. The relative configurations of the camporidines were determined by their H-H NOESY/ROESY and 1D NOE NMR correlations. The experimental ECD spectra of 1 and 2 were compared with their calculated ECD spectra to assign their absolute configurations. Camporidine A (1) displayed antimetastatic activity by suppression of cell invasion against the metastatic breast cancer cell line MDA-MB-231 and showed an anti-inflammatory effect by suppressing nitric oxide production induced by lipopolysaccharide. In addition, the putative biosynthetic gene cluster of the camporidines was identified, and the biosynthetic pathway of the camporidines was proposed based on bioinformatic analysis of the full genome of Streptomyces sp. STA1. Camporidines A and B (1 and 2) could be biosynthesized by a modular type I PKS containing an acyl transferase domain that accepts an unusual extender unit, which becomes the (C1'-C6') hexyl side chain. The post-PKS modification enzymes were predicted to perform an amination and an oxidation along with spontaneous Schiff base formation and generate the unique piperidine-cyclopentene-epoxide 6/5/3 tricyclic framework.

摘要

对 carpenter ant Camponotus kiusiuensis 的肠道细菌的化学研究导致了两种新生物碱,即来自 Streptomyces sp. STA1 的 camporidines A 和 B(1 和 2)的发现。基于 NMR 光谱和质谱分析,1 和 2 的结构被确定为具有哌啶-环戊烯-环氧化物 6/5/3 三环系统的新型聚酮生物碱。通过它们的 H-H NOESY/ROESY 和 1D NOE NMR 相关确定了 camporidines 的相对构型。通过比较实验 ECD 光谱和计算 ECD 光谱来确定 1 和 2 的绝对构型。Camporidine A(1)通过抑制转移性乳腺癌细胞系 MDA-MB-231 的细胞侵袭表现出抗转移活性,并通过抑制脂多糖诱导的一氧化氮产生表现出抗炎作用。此外,鉴定了 camporidines 的假定生物合成基因簇,并基于 Streptomyces sp. STA1 的全基因组的生物信息学分析提出了 camporidines 的生物合成途径。Camporidines A 和 B(1 和 2)可以通过包含酰基转移酶结构域的模块化 I 型 PKS 生物合成,该结构域接受不寻常的扩展单元,成为(C1'-C6')己基侧链。推测后 PKS 修饰酶沿自发席夫碱形成进行胺化和氧化,并产生独特的哌啶-环戊烯-环氧化物 6/5/3 三环骨架。

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