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基于与羊毛硫肽环化酶结构域相关肽段的计算分析对羊毛硫抗生素的产生及进化的见解

Insights into the production and evolution of lantibiotics from a computational analysis of peptides associated with the lanthipeptide cyclase domain.

作者信息

Maheshwari Nikunj, Jermiin Lars S, Cotroneo Chiara, Gordon Stephen V, Shields Denis C

机构信息

School of Medicine, University College Dublin, Dublin, Ireland.

Conway Institute of Biomolecular and Biomedical Research, University College Dublin, Dublin, Ireland.

出版信息

R Soc Open Sci. 2024 Jul 17;11(7):240491. doi: 10.1098/rsos.240491. eCollection 2024 Jul.

DOI:10.1098/rsos.240491
PMID:39021782
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11251773/
Abstract

Lanthipeptides are a large group of ribosomally encoded peptides cyclized by thioether and methylene bridges, which include the lantibiotics, lanthipeptides with antimicrobial activity. There are over 100 experimentally characterized lanthipeptides, with at least 25 distinct cyclization bridging patterns. We set out to understand the evolutionary dynamics and diversity of lanthipeptides. We identified 977 peptides in 2785 bacterial genomes from short open-reading frames encoding lanthipeptide modifiable amino acids (C, S and T) that lay chromosomally adjacent to genes encoding proteins containing the cyclase domain. These appeared to be synthesized by both known and novel enzymatic combinations. Our predictor of bridging topology suggested 36 novel-predicted topologies, including a single-cysteine topology seen in 179 lanthionine or labionin containing peptides, which were enriched for histidine. Evidence that supported the relevance of the single-cysteine containing lanthipeptide precursors included the presence of the labionin motif among single cysteine peptides that clustered with labionin-associated synthetase domains, and the leader features of experimentally defined lanthipeptides that were shared with single cysteine predictions. Evolutionary rate variation among peptide subfamilies suggests that selection pressures for functional change differ among subfamilies. Lanthipeptides that have recently evolved specific novel features may represent a richer source of potential novel antimicrobials, since their target species may have had less time to evolve resistance.

摘要

羊毛硫肽是一大类由硫醚桥和亚甲基桥环化的核糖体编码肽,其中包括羊毛硫抗生素,即具有抗菌活性的羊毛硫肽。目前已有100多种经过实验表征的羊毛硫肽,其环化桥接模式至少有25种不同类型。我们着手了解羊毛硫肽的进化动态和多样性。我们从2785个细菌基因组中鉴定出977种肽,这些肽来自短开放阅读框,编码可被修饰的羊毛硫肽氨基酸(C、S和T),它们在染色体上与编码含环化酶结构域蛋白质的基因相邻。这些肽似乎是由已知和新型的酶组合合成的。我们对桥接拓扑结构的预测器表明有36种新预测的拓扑结构,包括在179种含羊毛硫氨酸或拉比宁的肽中发现的单半胱氨酸拓扑结构,这些肽富含组氨酸。支持含单半胱氨酸羊毛硫肽前体相关性的证据包括,在与拉比宁相关合成酶结构域聚集的单半胱氨酸肽中存在拉比宁基序,以及与单半胱氨酸预测共享的实验确定的羊毛硫肽的前导特征。肽亚家族之间的进化速率差异表明,不同亚家族对功能变化的选择压力不同。最近进化出特定新特征的羊毛硫肽可能代表了更丰富的潜在新型抗菌剂来源,因为它们的目标物种可能没有那么多时间进化出抗性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/39d86aef7139/rsos.240491.f003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/83646a929af7/rsos.240491.f001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/ce3f8244fd0c/rsos.240491.f002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/39d86aef7139/rsos.240491.f003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/83646a929af7/rsos.240491.f001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/ce3f8244fd0c/rsos.240491.f002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f24/11251773/39d86aef7139/rsos.240491.f003.jpg

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