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首页> 外文期刊>MBio >A Genome-Wide Screen of Deletion Mutants in the Filamentous Saccharomyces?cerevisiae Background Identifies Ergosterol as a Direct Trigger of Macrophage Pyroptosis
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A Genome-Wide Screen of Deletion Mutants in the Filamentous Saccharomyces?cerevisiae Background Identifies Ergosterol as a Direct Trigger of Macrophage Pyroptosis

机译:丝状酿酒酵母背景中的缺失突变体的全基因组筛选背景确定麦角固醇是巨噬细胞凋亡的直接诱因。

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ABSTRACT Phagocytic cells such as macrophages play an important role in the host defense mechanisms mounted in response to the common human fungal pathogen Candida albicans . In vitro , C.?albicans triggers macrophage NLRP3- Casp1/11 -mediated pyroptosis, an inflammatory programmed cell death pathway. Here, we provide evidence that Casp1/11 -dependent pyroptosis occurs in the kidney of infected mice during the early stages of infection. We have also used a genome-wide screen of nonessential Σ1278b Saccharomyces cerevisiae genes to identify genes required for yeast-triggered macrophage pyroptosis. The set of genes identified by this screen was enriched for those with functions in lipid and sterol homeostasis and trafficking. These observations led us to discover that cell surface localization and/or total levels of ergosterol correlate with the ability of S.?cerevisiae , C.?albicans , and Cryptococcus?neoformans to trigger pyroptosis. Since the mammalian sterol cholesterol triggers NLRP3-mediated pyroptosis, we hypothesized that ergosterol may also do so. Consistent with that hypothesis, ergosterol-containing liposomes but not ergosterol-free liposomes induce pyroptosis. Cell wall mannoproteins directly bind ergosterol, and we found that Dan1, an ergosterol receptor mannoprotein, as well as specific mannosyltransferases, is required for pyroptosis, suggesting that cell wall-associated ergosterol may mediate the process. Taken together, these data indicate that ergosterol, like mammalian cholesterol, plays a direct role in yeast-mediated pyroptosis. IMPORTANCE Innate immune cells such as macrophages are key components of the host response to the human fungal pathogen Candida albicans . Macrophages undergo pyroptosis, an inflammatory, programmed cell death, in response to some species of pathogenic yeast. Prior to the work described in this report, yeast-triggered pyroptosis has been observed only in vitro ; here, we show that pyroptosis occurs in the initial stages of murine kidney infection, suggesting that it plays an important role in the initial response of the innate immune system to invasive yeast infection. We also show that a key component of the fungal plasma membrane, ergosterol, directly triggers pyroptosis. Ergosterol is also present in the fungal cell wall, most likely associated with mannoproteins, and is increased in hyphal cells compared to yeast cells. Our data indicate that specific mannoproteins are required for pyroptosis. This is consistent with a potential mechanism whereby ergosterol present in the outer mannoprotein layer of the cell wall is accessible to the macrophage-mediated process. Taken together, our data provide the first evidence that ergosterol plays a direct role in the host-pathogen interactions of fungi.
机译:摘要吞噬细胞(例如巨噬细胞)在应对常见的人类真菌病原体白色念珠菌的宿主防御机制中起着重要作用。在体外,白色念珠菌会触发巨噬细胞NLRP3- Casp1 / 11介导的凋亡,这是一种炎症性程序性细胞死亡途径。在这里,我们提供了证据,表明在感染的早期阶段,Casp1 / 11依赖的热凋亡发生在被感染小鼠的肾脏中。我们还使用了非必需Σ1278b酿酒酵母基因的全基因组筛选来鉴定酵母触发的巨噬细胞发烧症所需的基因。通过该筛选鉴定出的一组基因丰富了那些具有脂质和固醇稳态和运输功能的基因。这些发现使我们发现细胞表面的定位和/或麦角固醇的总水平与酿酒酵母,白色念珠菌和新球隐球菌引发焦磷酸化的能力有关。由于哺乳动物固醇胆固醇会触发NLRP3介导的凋亡,我们假设麦角固醇也可能会这样做。与该假设一致,含麦角固醇的脂质体而非不含麦角固醇的脂质体诱导焦磷酸化。细胞壁甘露糖蛋白直接结合麦角固醇,我们发现Dan1(一种麦角固醇受体甘露糖蛋白)以及特定的甘露糖基转移酶是热解所需的,这表明与细胞壁相关的麦角固醇可能介导了这一过程。综上所述,这些数据表明麦角固醇像哺乳动物的胆固醇一样,在酵母介导的细胞凋亡中起直接作用。重要信息先天性免疫细胞(例如巨噬细胞)是宿主对人类真菌病原体白色念珠菌反应的关键组成部分。巨噬细胞对某些种类的致病性酵母菌发生发烧,即炎症性程序性细胞死亡。在本报告中描述的工作之前,仅在体外观察到了酵母触发的热解。在这里,我们显示了热凋亡发生在鼠肾感染的初始阶段,这表明它在先天免疫系统对侵袭性酵母菌感染的初始应答中起着重要作用。我们还表明,真菌质膜的关键成分麦角固醇会直接引发焦磷酸化。麦角固醇也存在于真菌细胞壁中,最有可能与甘露糖蛋白有关,与酵母细胞相比,在菌丝细胞中麦角固醇的含量增加。我们的数据表明特定的甘露糖蛋白是焦磷酸化所必需的。这与潜在机制一致,由此巨噬细胞介导的过程可接近存在于细胞壁外部甘露糖蛋白层的麦角固醇。综上所述,我们的数据提供了麦角固醇在真菌的宿主-病原体相互作用中起直接作用的第一个证据。

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