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Signaling through IL-17C/IL-17RE Is Dispensable for Immunity to Systemic, Oral and Cutaneous Candidiasis

机译:通过IL-17C / IL-17RE进行信号传导可预防全身性,口腔和皮肤念珠菌病

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摘要

Copyright: © 2015 Conti et al. Candida albicans is a commensal fungal microbe of the human orogastrointestinal tract and skin. C . albicans causes multiple forms of disease in immunocompromised patients, including oral, vaginal, dermal and disseminated candidiasis. The cytokine IL-17 (IL-17A) and its receptor subunits, IL-17RA and IL-17RC, are required for protection to most forms of candidiasis. The importance of the IL-17R pathway has been observed not only in knockout mouse models, but also in humans with rare genetic mutations that impact generation of Th17 cells or the IL-17 signaling pathway, including Hyper-IgE Syndrome (STAT3 or TYK2 mutations) or IL17RA or ACT1 gene deficiency. The IL-17 family of cytokines is a distinct subclass of cytokines with unique structural and signaling properties. IL-17A is the bestcharacterized member of the IL-17 family to date, but far less is known about other IL-17-related cytokines. In this study, we sought to determine the role of a related IL-17 cytokine, IL-17C, in protection against oral, dermal and disseminated forms of C . albicans infection. IL-17C signals through a heterodimeric receptor composed of the IL-17RA and IL-17RE subunits. We observed that IL-17C mRNA was induced following oral C. albicans infection. However, mice lacking IL-17C or IL-17RE cleared C. albicans infections in the oral mucosa, skin and bloodstream at rates similar to WT littermate controls. Moreover, these mice demonstrated similar gene transcription profiles and recovery kinetics as WT animals. These findings indicate that IL-17C and IL-17RE are dispensable for immunity to the forms of candidiasis evaluated, and illustrate a surprisingly limited specificity of the IL-17 family of cytokines with respect to systemic, oral and cutaneous Candida infections.
机译:版权:©2015 Conti等。白色念珠菌是人类食道和皮肤的共生真菌。 C 。白色念珠菌在免疫功能低下的患者中引起多种疾病,包括口腔,阴道,皮肤和散发性念珠菌病。细胞因子IL-17(IL-17A)及其受体亚基IL-17RA和IL-17RC是保护大多数形式的念珠菌病所必需的。 IL-17R途径的重要性不仅在基因敲除的小鼠模型中得到了观察,而且在具有罕见基因突变的人类中也得到了观察,这些突变会影响Th17细胞或IL-17信号通路的产生,包括Hyper-IgE综合征(STAT3或TYK2突变) )或IL17RA或ACT1基因缺陷。 IL-17家族细胞因子是具有独特结构和信号传导特性的细胞因子的独特亚类。 IL-17A是迄今为止IL-17家族中最具特征的成员,但对其他IL-17相关细胞因子的了解却很少。在这项研究中,我们试图确定相关的IL-17细胞因子IL-17C在针对口服,皮肤和弥散性C的保护中的作用。白色念珠菌感染。 IL-17C通过由IL-17RA和IL-17RE亚基组成的异二聚体受体发出信号。我们观察到口服白色念珠菌感染后诱导IL-17C mRNA。但是,缺乏IL-17C或IL-17RE的小鼠清除了口腔粘膜,皮肤和血流中的白色念珠菌感染,其发生率与野生型同窝仔对照相似。此外,这些小鼠表现出与野生型动物相似的基因转录谱和恢复动力学。这些发现表明,IL-17C和IL-17RE对于针对所评估的念珠菌病形式的免疫力是必不可少的,并且说明了IL-17家族的细胞因子对全身,口腔和皮肤念珠菌感染的特异性出乎意料地有限。

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