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  1. National Taiwan Ocean University Research Hub
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請用此 Handle URI 來引用此文件: http://scholars.ntou.edu.tw/handle/123456789/17322
標題: Integrated Omics Strategy Reveals Cyclic Lipopeptides Empedopeptins from Massilia sp. YMA4 and Their Biosynthetic Pathway
作者: Ho, Shang-Tse
Ho, Ying-Ning 
Lin, Chih
Hsu, Wei-Chen
Lee, Han-Jung
Peng, Chia-Chi
Cheng, Han-Tan
Yang, Yu-Liang
關鍵字: Massilia;lipopeptides;biosynthesis;genome mining;metabolomics
公開日期: 四月-2021
出版社: MDPI
卷: 19
期: 4
來源出版物: MAR DRUGS
摘要: 
Empedopeptins-eight amino acid cyclic lipopeptides-are calcium-dependent antibiotics that act against Gram-positive bacteria such as Staphylococcus aureus by inhibiting cell wall biosynthesis. However, to date, the biosynthetic mechanism of the empedopeptins has not been well identified. Through comparative genomics and metabolomics analysis, we identified empedopeptin and its new analogs from a marine bacterium, Massilia sp. YMA4. We then unveiled the empedopeptin biosynthetic gene cluster. The core nonribosomal peptide gene null-mutant strains (Delta empC, Delta empD, and Delta empE) could not produce empedopeptin, while dioxygenase gene null-mutant strains (Delta empA and Delta empB) produced several unique empedopeptin analogs. However, the antibiotic activity of Delta empA and Delta empB was significantly reduced compared with the wild-type, demonstrating that the hydroxylated amino acid residues of empedopeptin and its analogs are important to their antibiotic activity. Furthermore, we found seven bacterial strains that could produce empedopeptin-like cyclic lipopeptides using a genome mining approach. In summary, this study demonstrated that an integrated omics strategy can facilitate the discovery of potential bioactive metabolites from microbial sources without further isolation and purification.
URI: http://scholars.ntou.edu.tw/handle/123456789/17322
ISSN: 1660-3397
DOI: 10.3390/md19040209
顯示於:海洋生物研究所
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