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IL-10 from regulatory T cells determines vaccine efficacy in murine Leishmania major infection.调节性T细胞产生的白细胞介素-10决定了小鼠利什曼原虫主要感染模型中的疫苗效力。
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Dendritic cell maturation by innate lymphocytes: coordinated stimulation of innate and adaptive immunity.天然淋巴细胞介导的树突状细胞成熟:天然免疫与适应性免疫的协同刺激
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The IL-6R alpha chain controls lung CD4+CD25+ Treg development and function during allergic airway inflammation in vivo.白细胞介素-6受体α链在体内变应性气道炎症期间控制肺CD4+CD25+调节性T细胞的发育和功能。
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白细胞介素-6和白细胞介素-12p40在介导抗杜氏利什曼原虫感染的保护作用及白细胞介素-10+ CD4+ T细胞扩增中的不同作用。

Distinct roles for IL-6 and IL-12p40 in mediating protection against Leishmania donovani and the expansion of IL-10+ CD4+ T cells.

作者信息

Stäger Simona, Maroof Asher, Zubairi Soombul, Sanos Stephanie L, Kopf Manfred, Kaye Paul M

机构信息

Immunology and Infection Unit, Hull York Medical School and Department of Biology, University of York, York, UK.

出版信息

Eur J Immunol. 2006 Jul;36(7):1764-71. doi: 10.1002/eji.200635937.

DOI:10.1002/eji.200635937
PMID:16791879
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2659577/
Abstract

Adoptive dendritic cell (DC) immunotherapy provides a useful experimental tool to evaluate immunoregulation in vivo and has previously been successfully used to enhance host resistance in a variety of experimental models of leishmaniasis. Here, we used this approach to identify IL-6 and IL-12p40 as critical cytokines that cooperate to mediate host protection to Leishmania donovani but which act independently to regulate expansion of IL-10(+) CD4(+) T cells, shown here for the first time to be associated with this infection. Adoptive transfer of LPS-activated bone marrow-derived DC (BMDC) from wild-type mice was therapeutically beneficial and led to enhanced resistance as measured by spleen parasite burden. In contrast, IL-6- or IL-12p40-deficient BMDC had no protective benefit, indicating that production of both cytokines was essential for the therapeutic efficacy of DC. IL-10 production by CD25(-) FoxP3(-) IL-10(+) CD4(+) T cells is a strong correlate of disease progression, and BMDC from wild-type mice inhibited expansion of these cells. Strikingly, IL-12-deficient BMDC could also inhibit the expansion of this T cell population whereas IL-6-deficient BMDC could not, indicating that IL-6 played a key role in this aspect of DC function in vivo. Breadth of cytokine production is thus an important factor when considering strategies for DC-based interventions.

摘要

过继性树突状细胞(DC)免疫疗法为评估体内免疫调节提供了一种有用的实验工具,并且此前已成功用于增强多种利什曼病实验模型中的宿主抵抗力。在此,我们采用这种方法确定白细胞介素-6(IL-6)和白细胞介素-12p40为关键细胞因子,它们协同介导宿主对杜氏利什曼原虫的保护作用,但在调节IL-10(+) CD4(+) T细胞的扩增方面独立发挥作用,本文首次表明这种T细胞与该感染有关。从野生型小鼠体内过继性转移脂多糖激活的骨髓来源的DC(BMDC)具有治疗益处,并通过脾脏寄生虫负荷测量显示出增强的抵抗力。相比之下,缺乏IL-6或IL-12p40的BMDC没有保护作用,这表明两种细胞因子的产生对于DC的治疗效果至关重要。CD25(-) FoxP3(-) IL-10(+) CD4(+) T细胞产生的IL-10与疾病进展密切相关,野生型小鼠的BMDC可抑制这些细胞的扩增。令人惊讶的是,缺乏IL-12的BMDC也能抑制这一T细胞群体的扩增,而缺乏IL-6的BMDC则不能,这表明IL-6在体内DC功能的这一方面起着关键作用。因此,在考虑基于DC的干预策略时,细胞因子产生的广度是一个重要因素。