The rational discovery of new specialized metabolites by genome mining represents a very promising strategy in the quest for new bioactive molecules. Ribosomally synthesized and post-translationally modified peptides (RiPPs) are a major class of natural product that derive from genetically encoded precursor peptides. However, RiPP gene clusters are particularly refractory to reliable bioinformatic predictions due to the absence of a common biosynthetic feature across all pathways. Here, we describe RiPPER, a new tool for the family-independent identification of RiPP precursor peptides and apply this methodology to search for novel thioamidated RiPPs in Actinobacteria. Until now, thioamidation was believed to be a rare post-translational modification, which is catalyzed by a pair of proteins (YcaO and TfuA) in Archaea. In Actinobacteria, the thioviridamide-like molecules are a family of cytotoxic RiPPs that feature multiple thioamides, which are proposed to be introduced by YcaO-TfuA proteins. Using RiPPER, we show that previously undescribed RiPP gene clusters encoding YcaO and TfuA proteins are widespread in Actinobacteria and encode a highly diverse landscape of precursor peptides that are predicted to make thioamidated RiPPs. To illustrate this strategy, we describe the first rational discovery of a new structural class of thioamidated natural products, the thiovarsolins from Streptomyces varsoviensis.
Uncovering the unexplored diversity of thioamidated ribosomal peptides in Actinobacteria using the RiPPER genome mining tool.
利用 RiPPER 基因组挖掘工具揭示放线菌中硫代酰胺化核糖体肽的未探索多样性
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作者:Santos-Aberturas Javier, Chandra Govind, Frattaruolo Luca, Lacret Rodney, Pham Thu H, Vior Natalia M, Eyles Tom H, Truman Andrew W
| 期刊: | Nucleic Acids Research | 影响因子: | 13.100 |
| 时间: | 2019 | 起止号: | 2019 May 21; 47(9):4624-4637 |
| doi: | 10.1093/nar/gkz192 | 研究方向: | 微生物学 |
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