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The Differentiation of CD4+ T-Helper Cell Subsets in the Context of Helminth Parasite Infection

机译:蠕虫寄生虫感染的背景下CD4 + T辅助细胞亚群的分化。

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摘要

Helminths are credited with being the major selective force driving the evolution of the so-called “type 2” immune responses in vertebrate animals, with their size and infection strategies presenting unique challenges to the immune system. Originally, type 2 immune responses were defined by the presence and activities of the CD4+ T-helper 2 subset producing the canonical cytokines IL-4, IL-5, and IL-13. This picture is now being challenged by the discovery of a more complex pattern of CD4+ T-helper cell subsets that appear during infection, including Tregs, Th17, Tfh, and more recently, Th22, Th9, and ThGM. In addition, a clearer view of the mechanisms by which helminths and their products selectively prime the CD4+ T-cell subsets is emerging. In this review, we have focused on recent data concerning the selective priming, differentiation, and functional role of CD4+ T-helper cell subsets in the context of helminth infection. We argue for a re-evaluation of the original Th2 paradigm and discuss how the observed plasticity of the T-helper subsets may enable the parasitized host to achieve an appropriate compromise between elimination, tissue repair, containment, and pathology.
机译:蠕虫被认为是驱动脊椎动物中所谓的“ 2型”免疫应答进化的主要选择力,它们的大小和感染策略对免疫系统提出了独特的挑战。最初,2型免疫应答是由CD4 + T-helper 2子集的存在和活性定义的,该子集产生典型的细胞因子IL-4,IL-5和IL-13。现在,发现在感染过程中出现的CD4 + T辅助细胞亚群的更复杂模式(包括Treg,Th17,Tfh,以及最近的Th22,Th9和ThGM。此外,关于蠕虫及其产物选择性引发CD4 + T细胞亚群的机制的清晰认识正在出现。在这篇综述中,我们集中于有关蠕虫感染背景下CD4 + T辅助细胞亚群的选择性启动,分化和功能作用的最新数据。我们主张对原始的Th2范式进行重新评估,并讨论观察到的T辅助亚型的可塑性如何使被寄生的宿主能够在消除,组织修复,遏制和病理之间取得适当的折衷。

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