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白蛋白能中和疏水毒素并调节致病性。

Albumin Neutralizes Hydrophobic Toxins and Modulates Pathogenicity.

机构信息

Department of Microbial Pathogenicity Mechanisms, Leibniz Institute for Natural Product Research and Infection Biology, Hans Knöll Institute, Jena, Germany.

Junior Research Group Adaptive Pathogenicity Strategies, Leibniz Institute for Natural Product Research and Infection Biology, Hans Knöll Institute, Jena, Germany.

出版信息

mBio. 2021 Jun 29;12(3):e0053121. doi: 10.1128/mBio.00531-21. Epub 2021 Jun 22.

Abstract

Albumin is abundant in serum but is also excreted at mucosal surfaces and enters tissues when inflammation increases vascular permeability. Host-associated opportunistic pathogens encounter albumin during commensalism and when causing infections. Considering the ubiquitous presence of albumin, we investigated its role in the pathogenesis of infections with the model human fungal pathogen, Candida albicans. Albumin was introduced in various models that mimic different stages of systemic or mucosal candidiasis, where it reduced the ability of C. albicans to damage host cells. The amphipathic toxin candidalysin mediates necrotic host cell damage induced by C. albicans. Using cellular and biophysical assays, we determined that albumin functions by neutralizing candidalysin through hydrophobic interactions. We discovered that albumin, similarly, can neutralize a variety of fungal (α-amanitin), bacterial (streptolysin O and staurosporin), and insect (melittin) hydrophobic toxins. These data suggest albumin as a defense mechanism against toxins, which can play a role in the pathogenesis of microbial infections. Albumin is the most abundant serum protein in humans. During inflammation, serum albumin levels decrease drastically, and low albumin levels are associated with poor patient outcome. Thus, albumin may have specific functions during infection. Here, we describe the ability of albumin to neutralize hydrophobic microbial toxins. We show that albumin can protect against damage induced by the pathogenic yeast C. albicans by neutralizing its cytolytic toxin candidalysin. These findings suggest that albumin is a toxin-neutralizing protein that may play a role during infections with toxin-producing microorganisms.

摘要

血清中富含白蛋白,但也会从黏膜表面排泄,并且在炎症增加血管通透性时进入组织。宿主相关的机会性病原体在共生和引起感染时会遇到白蛋白。考虑到白蛋白的普遍存在,我们研究了它在人类真菌病原体白色念珠菌感染发病机制中的作用。白蛋白被引入了各种模拟系统性或黏膜念珠菌病不同阶段的模型中,在这些模型中,它降低了白色念珠菌损伤宿主细胞的能力。两亲性毒素白色念珠菌溶素介导白色念珠菌引起的宿主细胞坏死损伤。通过细胞和生物物理测定,我们确定白蛋白通过疏水相互作用来中和白色念珠菌溶素。我们发现白蛋白同样可以中和各种真菌(α-鹅膏蕈碱)、细菌(链球菌溶血素 O 和星孢菌素)和昆虫(蜂毒素)的疏水毒素。这些数据表明白蛋白作为一种针对毒素的防御机制,可能在微生物感染的发病机制中发挥作用。白蛋白是人类血清中最丰富的蛋白质。在炎症期间,血清白蛋白水平急剧下降,低白蛋白水平与患者预后不良有关。因此,白蛋白在感染期间可能具有特定的功能。在这里,我们描述了白蛋白中和疏水微生物毒素的能力。我们表明,白蛋白可以通过中和其细胞溶解毒素白色念珠菌溶素来保护免受致病性酵母白色念珠菌诱导的损伤。这些发现表明白蛋白是一种中和毒素的蛋白质,可能在产毒素微生物感染期间发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/af55/8262992/957d2cc9ff25/mbio.00531-21-f001.jpg

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