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首页> 外文期刊>Applied and Environmental Microbiology >Discovery of a New Source of Rifamycin Antibiotics in Marine Sponge Actinobacteria by Phylogenetic Prediction
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Discovery of a New Source of Rifamycin Antibiotics in Marine Sponge Actinobacteria by Phylogenetic Prediction

机译:通过系统发育预测在海洋海绵放线菌中发现利福霉素抗生素的新来源

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摘要

Phylogenetic analysis of the ketosynthase (KS) gene sequences of marine sponge-derived Salinispora strains of actinobacteria indicated that the polyketide synthase (PKS) gene sequence most closely related to that of Salinispora was the rifamycin B synthase of Amycolatopsis mediterranei. This result was not expected from taxonomic species tree phylogenetics using 16S rRNA sequences. From the PKS sequence data generated from our sponge-derived Salinispora strains, we predicted that such strains might synthesize rifamycin-like compounds. Liquid chromatography-tandem mass spectrometry (LC/MS/MS) analysis was applied to one sponge-derived Salinispora strain to test the hypothesis of rifamycin synthesis. The analysis reported here demonstrates that this Salinispora isolate does produce compounds of the rifamycin class, including rifamycin B and rifamycin SV. A rifamycin-specific KS primer set was designed, and that primer set increased the number of rifamycin-positive strains detected by PCR screening relative to the number detectable using a conserved KS-specific set. Thus, the Salinispora group of actinobacteria represents a potential new source of rifamycins outside the genus Amycolatopsis and the first recorded source of rifamycins from marine bacteria.
机译:对海洋海绵来源的放线杆菌的沙里氏菌菌株的酮合酶(KS)基因序列进行系统进化分析表明,与沙里氏菌最密切相关的聚酮化合物合酶(PKS)基因序列是地中海扁桃体的利福霉素B合酶。使用16S rRNA序列从分类学物种树系统发育学中无法预期到该结果。根据从我们的海绵沙门氏菌菌株产生的PKS序列数据,我们预测此类菌株可能合成利福霉素样化合物。将液相色谱-串联质谱(LC / MS / MS)分析应用于一种海绵衍生的沙利氏菌菌株,以检验利福霉素合成的假说。此处报道的分析表明,这种盐霉菌分离物确实产生了利福霉素类化合物,包括利福霉素B和利福霉素SV。设计了利福霉素特异性KS引物组,该引物组相对于使用保守的KS特异性组可检测的数目,增加了通过PCR筛选检测到的利福霉素阳性菌株的数目。因此,放线菌的Salinispora组代表了除真菌病菌之外的利福霉素的潜在新来源,也是海洋细菌中利福霉素的第一个记录来源。

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