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首页> 外文期刊>Clinical and vaccine immunology: CVI >Interleukin 1 (IL-1)- and IL-23-Mediated Expansion of Filarial Antigen-Specific Th17 and Th22 Cells in Filarial Lymphedema
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Interleukin 1 (IL-1)- and IL-23-Mediated Expansion of Filarial Antigen-Specific Th17 and Th22 Cells in Filarial Lymphedema

机译:白介素1(IL-1) - 和IL-23介导的丝状抗原特异性Th17和Th22细胞在丝状淋巴水肿中的膨胀

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摘要

Lymphatic filarial disease is known to be associated with elevated Th1 responses and normal or diminished Th2 responses to parasite-specific antigens. The roles of Th17 cells and the recently described Th22 cells have not been examined in detail in either filarial infection itself or in filarial disease (e. g., lymphedema and elephantiasis). To explore the roles of Th17 and Th22 cells and their subsets, we examined the frequencies of these cells in individuals with filarial lymphedema (chronic pathology [CP]), in clinically asymptomatic infected (INF) individuals, and in uninfected (UN) individuals ex vivo and in response to parasite and nonparasite antigens. Those with disease (CP) had significantly expanded frequencies of Th17 and Th22 cells, compared with either INF or UN individuals, at baseline (ex vivo) and in response to parasite antigens. This antigen-driven expansion of Th17 and Th22 cells was dependent on interleukin 1 (IL-1), IL-23, and, to lesser extent, transforming growth factor beta (TGF-beta), as blockade of any of these cytokines resulted in significantly diminished frequencies of Th17 and Th22 cells. Our findings, therefore, suggest that filarial parasite-driven expansion of Th17 and Th22 cells is associated with the pathogenesis of filarial infections and disease.
机译:已知淋巴丝状疾病与TH1反应升高以及对寄生虫特异性抗原的正常反应有关。尚未在丝状感染本身或丝状疾病中详细检查Th17细胞和最近描述的Th22细胞的作用(例如,淋巴水肿和脂肪症)。为了探索Th17和Th22细胞及其子集的作用,我们检查了这些细胞在丝状淋巴水肿(慢性病理[CP])中,临床无症状感染(INF)个体以及未感染的(UN)个体中的这些细胞的频率(慢性病理[CP])体内以及响应寄生虫和非寄生虫抗原。与INF或联合国个体相比,基线(Ex ex vivo)和对寄生虫抗原的响应,患有疾病(CP)的Th17和Th22细胞的频率显着扩大。 Th17和Th22细胞的这种抗原驱动的膨胀取决于白介素1(IL-1),IL-23,以及在较小程度上转化生长因子β(TGF-BETA),这是对这些细胞因子中任何一个的阻塞,从而导致了这些细胞因子的阻塞Th17和Th22细胞的频率显着降低。因此,我们的发现表明,Th17和Th22细胞的丝状寄生虫驱动的膨胀与丝状感染和疾病的发病机理有关。

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