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弗氏菌素 C-G,链霉菌 RM-4-15 产生的吡喃萘醌。

Frenolicins C-G, pyranonaphthoquinones from Streptomyces sp. RM-4-15.

机构信息

Center for Pharmaceutical Research and Innovation, College of Pharmacy, University of Kentucky, 789 South Limestone Street, Lexington, Kentucky 40536-0596, USA.

出版信息

J Nat Prod. 2013 Aug 23;76(8):1441-7. doi: 10.1021/np400231r. Epub 2013 Aug 14.

Abstract

Appalachian active coal fire sites were selected for the isolation of bacterial strains belonging to the class actinobacteria. A comparison of high-resolution electrospray ionization mass spectrometry (HRESIMS) and ultraviolet (UV) absorption profiles from isolate extracts to natural product databases suggested Streptomyces sp. RM-4-15 to produce unique metabolites. Four new pyranonaphthoquinones, frenolicins C-F (1-4), along with three known analogues, frenolicin (6), frenolicin B (7), and UCF76-A (8), were isolated from the fermentation of this strain. An additional new analogue, frenolicin G (5), along with two known compounds, deoxyfrenolicin (9) and UCF 13 (10), were isolated from the fermentation supplied with 18 mg/L of scandium chloride, the first example, to the best of our knowledge, wherein scandium chloride supplementation led to the confirmed production of new bacterial secondary metabolites. Structures 1-5 were elucidated on the basis of spectral analysis and chemical modification. While frenolicins are best known for their anticoccidial activity, the current study revealed compounds 6-9 to exhibit moderate cytotoxicity against the human lung carcinoma cell line (A549) and thereby extends the anticancer SAR for this privileged scaffold.

摘要

阿巴拉契亚活性煤火地区被选为分离属于放线菌纲的细菌菌株。将分离物提取物的高分辨电喷雾电离质谱 (HRESIMS) 和紫外 (UV) 吸收图谱与天然产物数据库进行比较,表明链霉菌 RM-4-15 产生独特的代谢物。从该菌株的发酵中分离得到了四个新的吡喃萘醌, frenolicins C-F(1-4),以及三个已知的类似物, frenolicin(6),frenolicin B(7)和 UCF76-A(8)。此外,还从添加了 18mg/L 氯化钪的发酵液中分离得到了 frenolicin G(5),以及两个已知化合物 deoxyfrenolicin(9)和 UCF 13(10),这是迄今为止首次证明氯化钪补充导致新的细菌次生代谢物的确认生产。根据光谱分析和化学修饰,确定了结构 1-5。虽然 frenolicins 以其抗球虫活性而闻名,但目前的研究表明,化合物 6-9 对人肺癌细胞系(A549)表现出中等的细胞毒性,从而扩展了该特权支架的抗癌 SAR。

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