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功能影响金黄色葡萄球菌细胞群体随时间的遗传变化。

Functional Influences Genetic Changes within a Staphylococcus aureus Cell Population over Time.

机构信息

Department of Molecular and Biomedical Sciences, School of Biological Sciences, The University of Adelaidegrid.1010.0, Adelaide, South Australia, Australia.

Research Centre for Infectious Disease (RCID), The University of Adelaidegrid.1010.0, Adelaide, South Australia, Australia.

出版信息

J Bacteriol. 2022 Oct 18;204(10):e0013822. doi: 10.1128/jb.00138-22. Epub 2022 Sep 26.

Abstract

Prolonged survival in the host-bacteria microenvironment drives the selection of alternative cell types in Staphylococcus aureus, permitting quasi-dormant sub-populations to develop. These facilitate antibiotic tolerance, long-term growth, and relapse of infection. Small Colony Variants (SCV) are an important cell type associated with persistent infection but are difficult to study due to the instability of the phenotype and reversion to the normal cell type. We have previously reported that under conditions of growth in continuous culture over a prolonged culture time, SCVs dominated a heterogenous population of cell types and these SCVs harbored a mutation in the DNA binding domain of the gene for the transcription factor, . To investigate this specific cell type further, S. aureus WCH-SK2-Δ itself was assessed with continuous culture. Compared to the wild type, the mutant strain required fewer generations to select for SCVs. There was an increased rate of mutagenesis within the Δ strain compared to the wild type, which we postulate is the mechanism explaining the increased emergence of SCV selection. The derived SCVs had impeded metabolism, altered MIC to specific antibiotics and an increased biofilm formation compared to non-SCV strain. Whole genomic sequencing detected single nucleotide polymorphisms (SNP) in phosphoglucosamine mutase and tyrosine recombinase . In addition, several genomic rearrangements were detected which affected genes involved in important functions such as antibiotic and toxic metal resistance and pathogenicity. Thus, we propose a direct link between and the SCV phenotype. Within a bacterial population, a stochastically generated heterogeneity of phenotypes allows continual survival against current and future stressors. The generation of a sub-population of quasi-dormant Small Colony Variants (SCV) in Staphylococcus aureus is such a mechanism, allowing for persistent or relapse of infection despite initial intervention seemingly clearing the infection. The use of continuous culture under clinically relevant conditions has allowed us to introduce time to the growth system and selects SCV within the population. This study provides valuable insights into the generation of SCV which are not addressed in standard laboratory generated models and reveals new pathways for understanding persistent S. aureus infection which can potentially be targeted in future treatments of persistent S. aureus infection.

摘要

在宿主-细菌微环境中的长期存活促使金黄色葡萄球菌选择替代细胞类型,从而使准休眠亚群得以发展。这些细胞类型促进了抗生素耐受性、长期生长和感染复发。小菌落变异体(SCV)是与持续性感染相关的重要细胞类型,但由于表型的不稳定性和向正常细胞类型的回复,因此难以研究。我们之前曾报道过,在长时间连续培养的条件下,SCV 在异质细胞群体中占主导地位,并且这些 SCV 携带转录因子基因的 DNA 结合结构域突变。为了进一步研究这种特定的细胞类型,我们对金黄色葡萄球菌 WCH-SK2-Δ 本身进行了连续培养评估。与野生型相比,Δ 突变株需要更少的代次来选择 SCV。与野生型相比,Δ 株的突变率增加,我们推测这是解释 SCV 选择增加的机制。与非-SCV 菌株相比,Δ 衍生的 SCV 代谢受到阻碍,对特定抗生素的 MIC 发生改变,生物膜形成增加。全基因组测序检测到磷酸葡萄糖胺变位酶和酪氨酸重组酶的单核苷酸多态性(SNP)。此外,还检测到了几个基因组重排,这些重排影响了参与抗生素和有毒金属抗性以及致病性等重要功能的基因。因此,我们提出了 与 SCV 表型之间的直接联系。在细菌群体中,表型的随机异质性允许其持续生存,以应对当前和未来的应激源。金黄色葡萄球菌中准休眠小菌落变异体(SCV)亚群的产生就是这样一种机制,尽管最初的干预似乎清除了感染,但仍允许持续性或感染复发。在临床相关条件下使用连续培养使我们能够在生长系统中引入时间,并在种群中选择 SCV。这项研究为 SCV 的产生提供了有价值的见解,这些见解在标准实验室产生的模型中没有得到解决,并揭示了理解金黄色葡萄球菌持续性感染的新途径,这些途径可能成为未来治疗金黄色葡萄球菌持续性感染的靶点。

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