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Cytotoxic alkaloids from the marine shellfish-associated fungus Aspergillus sp. XBB-4 induced by an amino acid-directed strategy

机译:来自海洋贝类相关真菌的细胞毒性生物碱曲霉属。由氨基酸导向策略引起的XBB-4

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摘要

Eight different culture media were used to culture shellfish Panopea abbreviate associated fungus Aspergillus sp. XBB-4. In a glucose-peptone-yeast (GPY) culture medium supplied with amino acids, this fungus can produce chemodiversity metabolites. Four new alkaloids including three β-carboline alkaloids, aspercarbolines A–C ( 1–3 ) and one piperazinedione, asperdione A ( 13 ) along with nine known compounds were isolated. The structures were elucidated mainly based on the NMR, MS, ECD and X-ray single-crystal diffraction data. The possible biosynthetic pathways of aspercarbolines A–C ( 1–3 ) were proposed. All compounds ( 1–13 ) were evaluated for their cytotoxicity against six cancer cell lines, including human nasopharyngeal carcinoma cell lines CNE1, CNE2, HONE1 and SUNE1, and human hepatocellular carcinoma cell lines hepG2 and QGY7701.
机译:八种不同的培养基用于培养贝类Panopea缩写相关的真菌Aspergillus sp。 XBB-4。在供应氨基酸的葡萄糖蛋白酵母(GPY)培养基中,该真菌可以产生化学大学代谢物。四种新的生物碱,包括三个β-咔啉生物碱,Asparboline A-C(1-3)和一个哌嗪,Asperdione A(13)以及九个已知化合物。主要基于NMR,MS,ECD和X射线单晶衍射数据来阐明该结构。提出了Asparboline A-C(1-3)的可能的生物合成途径。所有化合物(1-13)均针对六种癌细胞系评价其细胞毒性,包括人类鼻咽癌细胞系CNE1,CNE2,Hone1和Sune1和人肝细胞癌细胞系HepG2和QGy7701。

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