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An improved method for specificity annotation shows a distinct evolutionary divergence among the microbial enzymes of the cholylglycine hydrolase family

机译:一种改进的特异性注释方法显示了硫甘氨酸水解酶系列的微生物酶的不同进化分歧

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Bile salt hydrolases (BSHs) are gut microbial enzymes that play a significant role in the bile acid modification pathway. Penicillin V acylases (PVAs) are enzymes produced by environmental microbes, having a possible role in pathogenesis or scavenging of phenolic compounds in their microbial habitats. The correct annotation of such physiologically and industrially important enzymes is thus vital. The current methods relying solely on sequence homology do not always provide accurate annotations for these two members of the cholylglycine hydrolase (CGH) family as BSH/PVA enzymes. Here, we present an improved method [binding site similarity (BSS)-based scoring system] for the correct annotation of the CGH family members as BSH/PVA enzymes, which along with the phylogenetic information incorporates the substrate specificity as well as the binding site information. The BSS scoring system was developed through the analysis of the binding sites and binding modes of the available BSH/PVA structures with substrates glycocholic acid and penicillin V. The 198 sequences in the dataset were then annotated accurately using BSS scores as BSH/PVA enzymes. The dataset presented contained sequences from Gram-positive bacteria, Gram-negative bacteria and archaea. The clustering obtained for the dataset using the method described above showed a clear distinction in annotation of Gram-positive bacteria and Gram-negative bacteria. Based on this clustering and a detailed analysis of the sequences of the CGH family in the dataset, we could infer that the CGH genes might have evolved in accordance with the hypothesis stating the evolution of diderms and archaea from the monoderms.
机译:胆汁盐水解酶(BSH)是在胆汁酸改性途径中起显着作用的肠道微生物酶。青霉素V酰基酶(PVA)是环境微生物产生的酶,其在其微生物栖息地中的发病机制或清除酚类化合物的发病作用。因此,这种生理学和工业上重要的酶的正确注释是至关重要的。仅仅对序列同源性依赖的目前的方法并不总是为胆甘氨酸水解酶(CGH)系列的这两个成员作为BSH / PVA酶提供准确的注释。在这里,我们提出了一种改进的方法[结合位点相似性(BSS)的评分系统],用于将CGH系列成员作为BSH / PVA酶的正确注释,与系统发育信息掺入底物特异性以及结合位点信息。 BSS评分系统是通过分析底物甘油酸和青霉素V的可用BSH / PVA结构的结合位点和结合模式而开发的。然后使用BSS分数作为BSH / PVA酶准确地注释数据集中的198序列。该数据集呈现含有革兰氏阳性细菌,革兰氏阴性细菌和古痤疮的序列。使用上述方法对数据集获得的聚类显示出在革兰氏阳性细菌和革兰氏阴性细菌的注释中的明显区别。基于该聚类和对数据集中的CGH系列序列的详细分析,我们可以推断CGH基因可能根据假设阐述了从单胚层的迪特氏和古代的演变。

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