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比较琼氏不动杆菌和其他不动杆菌属物种的基因组特征和次生代谢物生物合成潜力。

Comparative genome features and secondary metabolite biosynthetic potential of Kutzneria chonburiensis and other species of the genus Kutzneria.

机构信息

Department of Microbiology, Faculty of Public Health, Mahidol University, Bangkok, 10400, Thailand.

Omics Sciences and Bioinformatics Center, Faculty of Science, Chulalongkorn University, Bangkok, 10330, Thailand.

出版信息

Sci Rep. 2023 May 31;13(1):8794. doi: 10.1038/s41598-023-36039-x.

Abstract

Actinobacteria are well known as a rich source of diversity of bioactive secondary metabolites. Kutzneria, a rare actinobacteria belonging to the family Pseudonocardiaceae has abundance of secondary metabolite biosynthetic gene clusters (BGCs) and is one of important source of natural products and worthy of priority investigation. Currently, Kutzneria chonburiensis SMC256 has been the latest type-strain of the genus and its genome sequence has not been reported yet. Therefore, we present the first report of new complete genome sequence of SMC256 (genome size of 10.4 Mbp) with genome annotation and feature comparison between SMC256 and other publicly available Kutzneria species. The results from comparative and functional genomic analyses regarding the phylogenomic and the clusters of orthologous groups of proteins (COGs) analyses indicated that SMC256 is most closely related to Kutzneria sp. 744, Kutzneria kofuensis, Kutzneria sp. CA-103260 and Kutzneria buriramensis. Furthermore, a total of 322 BGCs were also detected and showed diversity among the Kutzneria genomes. Out of which, 38 clusters showing the best hit to the most known BGCs were predicted in the SMC256genome. We observed that six clusters responsible for biosynthesis of antimicrobials/antitumor metabolites were strain-specific in Kutzneria chonburiensis. These putative metabolites include virginiamycin S1, lysolipin I, esmeraldin, rakicidin, aclacinomycin and streptoseomycin. Based on these findings, the genome of Kutzneria chonburiensis contains distinct and unidentified BGCs different from other members of the genus, and the use of integrative genomic-based approach would be a useful alternative effort to target, isolate and identify putative and undiscovered secondary metabolites suspected to have new and/or specific bioactivity in the Kutzneria.

摘要

放线菌是生物活性次生代谢物多样性的丰富来源。Kutzneria 是一种罕见的放线菌,属于拟诺卡氏菌科,其次生代谢物生物合成基因簇 (BGCs) 丰富,是天然产物的重要来源之一,值得优先研究。目前,Kutzneria chonburiensis SMC256 是该属的最新模式株,但尚未报道其基因组序列。因此,我们首次报道了 SMC256 的完整基因组序列(基因组大小为 10.4 Mbp),并进行了基因组注释和与其他公开的 Kutzneria 物种的特征比较。基于系统发育和直系同源基因簇 (COGs) 的比较和功能基因组分析结果表明,SMC256 与 Kutzneria sp. 744、Kutzneria kofuensis、Kutzneria sp. CA-103260 和 Kutzneria buriramensis 最为密切相关。此外,还检测到总共 322 个 BGCs,并且在 Kutzneria 基因组之间显示出多样性。其中,在 SMC256 基因组中预测了 38 个显示与最知名 BGCs 最佳匹配的簇。我们观察到,在 Kutzneria chonburiensis 中,有六个负责合成抗菌/抗肿瘤代谢物的簇是菌株特异性的。这些推定的代谢物包括 virginiamycin S1、lysolipin I、esmeraldin、rakicidin、aclacinomycin 和 streptoseomycin。基于这些发现,Kutzneria chonburiensis 的基因组包含与该属其他成员不同的独特和未识别的 BGCs,并且基于整合基因组的方法将是一种有用的替代方法,以靶向、分离和鉴定疑似具有新的和/或特定生物活性的假定和未发现的次生代谢物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eac5/10232511/81db47285f74/41598_2023_36039_Fig1_HTML.jpg

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