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Exploring the mechanisms of action of human secretory RNase 3 and RNase 7 against Candida albicans.

机译:探索人类分泌性RNase 3和RNase 7对白色念珠菌的作用机制。

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摘要

Human antimicrobial RNases, which belong to the vertebrate RNase A superfamily and are secreted upon infection, display a wide spectrum of antipathogen activities. In this work, we examined the antifungal activity of the eosinophil RNase 3 and the skin-derived RNase 7, two proteins expressed by innate cell types that are directly involved in the host defense against fungal infection. Candida albicans has been selected as a suitable working model for testing RNase activities toward a eukaryotic pathogen. We explored the distinct levels of action of both RNases on yeast by combining cell viability and membrane model assays together with protein labeling and confocal microscopy. Site-directed mutagenesis was applied to ablate either the protein active site or the key anchoring region for cell binding. This is the first integrated study that highlights the RNases’ dual mechanism of action. Along with an overall membrane-destabilization process, the RNases could internalize and target cellular RNA. The data support the contribution of the enzymatic activity for the antipathogen action of both antimicrobial proteins, which can be envisaged as suitable templates for the development of novel antifungal drugs. We suggest that both human RNases work as multitasking antimicrobial proteins that provide a first line immune barrier.
机译:属于脊椎动物RNase A超家族的人抗菌RNase表现出广泛的抗病原菌活性,它们在感染时会分泌出来。在这项工作中,我们检查了嗜酸性粒细胞RNase 3和皮肤来源的RNase 7的抗真菌活性,这是先天细胞类型表达的两种蛋白,它们直接参与宿主对抗真菌感染的防御作用。白色念珠菌已被选作测试RNase对真核病原体活性的合适工作模型。我们通过结合细胞活力和膜模型测定以及蛋白质标记和共聚焦显微镜研究了两种核糖核酸酶对酵母的不同作用水平。应用定点诱变消融蛋白质活性位点或细胞结合的关键锚定区。这是第一项强调RNase双重作用机制的综合研究。连同整个膜去稳定化过程,RNase可以内化并靶向细胞RNA。数据支持了酶活性对两种抗菌蛋白的抗病原作用的贡献,可以将其设想为开发新型抗真菌药物的合适模板。我们建议这两种人类RNase都可以作为多任务抗菌蛋白,提供一线免疫屏障。

著录项

  • 作者

    Salazar Vivian A.;

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  • 年度 2016
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  • 原文格式 PDF
  • 正文语种 eng
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