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在类人体皮肤环境中的调控程序。

The regulatory program in a human skin-like environment.

机构信息

Department of Immunology and Microbiology, University of Colorado Anschutz Medical Campus, Aurora, Colorado, USA.

Department of Veterans Affairs, Eastern Colorado Healthcare System, Aurora, Colorado, USA.

出版信息

mBio. 2024 May 8;15(5):e0045324. doi: 10.1128/mbio.00453-24. Epub 2024 Mar 28.

Abstract

UNLABELLED

is a Gram-positive pathogen responsible for the majority of skin and soft tissue infections (SSTIs). colonizes the anterior nares of approximately 20%-30% of the population and transiently colonizes the skin, thereby increasing the risk of developing SSTIs and more serious infections. Current laboratory models that mimic the skin surface environment are expensive, require substantial infrastructure, and limit the scope of bacterial physiology studies under human skin conditions. To overcome these limitations, we developed a cost-effective, open-source, chemically defined media recipe termed skin-like medium (SLM) that incorporates key aspects of the human skin surface environment and supports growth of several staphylococcal species. We utilized SLM to investigate the transcriptional response of methicillin-resistant (MRSA) following growth in SLM compared to a commonly used laboratory media. Through RNA-seq analysis, we observed the upregulation of several virulence factors, including genes encoding functions involved in adhesion, proteolysis, and cytotoxicity. To further explore these findings, we conducted quantitative reverse transcription-PCR (qRT-PCR) experiments to determine the influence of media composition, pH, and temperature on the transcriptional response of key factors involved in adhesion and virulence. We also demonstrated that MRSA primed in SLM adhered better to human corneocytes and demonstrated adhesin-specific phenotypes that previously required genetic manipulation. This improved adherence to corneocytes was dependent on both acidic pH and growth in SLM. These results support the potential utility of SLM as an model for assessing staphylococcal physiology and metabolism on human skin.

IMPORTANCE

is the major cause of skin diseases, and its increased prevalence in skin colonization and infections present a need to understand its physiology in this environment. The work presented here outlines upregulation of colonization and virulence factors using a newly developed medium that strives to replicate the human skin surface environment and demonstrates roles for adhesins clumping factor A (ClfA), serine-rich repeat glycoprotein adhesin (SraP), and the fibronectin binding proteins (Fnbps) in human corneocyte adherence.

摘要

未加标签

是一种革兰氏阳性病原体,负责大多数皮肤和软组织感染(SSTIs)。它定植于大约 20%-30%人口的前鼻孔,并短暂定植于皮肤,从而增加了发生 SSTIs 和更严重感染的风险。目前模仿皮肤表面环境的实验室模型昂贵、需要大量基础设施,并限制了在人体皮肤条件下研究细菌生理学的范围。为了克服这些限制,我们开发了一种经济高效、开源、化学定义的培养基配方,称为皮肤样培养基(SLM),它包含了人类皮肤表面环境的关键方面,并支持几种葡萄球菌物种的生长。我们利用 SLM 研究了耐甲氧西林金黄色葡萄球菌(MRSA)在 SLM 中生长与在常用实验室培养基中生长相比的转录反应。通过 RNA-seq 分析,我们观察到了几个毒力因子的上调,包括编码与粘附、蛋白水解和细胞毒性有关的功能的基因。为了进一步探讨这些发现,我们进行了定量逆转录-PCR(qRT-PCR)实验,以确定培养基组成、pH 值和温度对粘附和毒力相关关键因素转录反应的影响。我们还表明,在 SLM 中预培养的 MRSA 粘附到人类角质细胞的能力更好,并表现出以前需要遗传操作的粘附素特异性表型。这种对角质细胞的粘附增强依赖于酸性 pH 值和在 SLM 中的生长。这些结果支持 SLM 作为评估金黄色葡萄球菌在人体皮肤生理学和新陈代谢的模型的潜在用途。

重要性

是皮肤病的主要原因,其在皮肤定植和感染中的增加患病率需要了解其在这种环境中的生理学。这里介绍的工作使用一种新开发的培养基上调了定植和毒力因子的表达,该培养基旨在复制人类皮肤表面环境,并证明了凝聚因子 A(ClfA)、丝氨酸丰富重复糖蛋白粘附素(SraP)和纤维结合蛋白(Fnbps)在人类角质细胞粘附中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2752/11077960/aa5c571d360a/mbio.00453-24.f001.jpg

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