首页> 美国卫生研究院文献>The Journal of Experimental Medicine >CD40L+ CD4+ memory T cells migrate in a CD62P-dependent fashion into reactive lymph nodes and license dendritic cells for T cell priming
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CD40L+ CD4+ memory T cells migrate in a CD62P-dependent fashion into reactive lymph nodes and license dendritic cells for T cell priming

机译:CD40L + CD4 +记忆T细胞以CD62P依赖性方式迁移到反应性淋巴结并许可树突状细胞用于T细胞启动

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摘要

There is growing evidence that the maturation state of dendritic cells (DCs) is a critical parameter determining the balance between tolerance and immunity. We report that mouse CD4+ effector memory T (TEM) cells, but not naive or central memory T cells, constitutively expressed CD40L at levels sufficient to induce DC maturation in vitro and in vivo in the absence of antigenic stimulation. CD4+ TEM cells were excluded from resting lymph nodes but migrated in a CD62P-dependent fashion into reactive lymph nodes that were induced to express CD62P, in a transient or sustained fashion, on high endothelial venules. Trafficking of CD4+ TEM cells into chronic reactive lymph nodes maintained resident DCs in a mature state and promoted naive T cell responses and experimental autoimmune encephalomyelitis (EAE) to antigens administered in the absence of adjuvants. Antibodies to CD62P, which blocked CD4+ TEM cell migration into reactive lymph nodes, inhibited DC maturation, T cell priming, and induction of EAE. These results show that TEM cells can behave as endogenous adjuvants and suggest a mechanistic link between lymphocyte traffic in lymph nodes and induction of autoimmunity.
机译:越来越多的证据表明,树突状细胞(DC)的成熟状态是决定耐受性和免疫力之间平衡的关键参数。我们报告说,小鼠CD4 + 效应记忆T(TEM)细胞,而非幼稚或中央记忆T细胞,组成型表达CD40L,其水平足以在缺乏抗原性的情况下在体外和体内诱导DC成熟。刺激。 CD4 + TEM细胞从静息淋巴结中排除,但以CD62P依赖性的方式迁移到反应性淋巴结,这些淋巴结被诱导以短暂或持续的方式在高内皮小静脉上表达CD62P。将CD4 + TEM细胞贩运到慢性反应性淋巴结中,可将常驻DC维持在成熟状态,并促进对未使用佐剂时施用的抗原的幼稚T细胞反应和实验性自身免疫性脑脊髓炎(EAE)。 CD62P抗体可阻止CD4 + TEM细胞迁移至反应性淋巴结,抑制DC成熟,T细胞启动和诱导EAE。这些结果表明,TEM细胞可以作为内源性佐剂,提示淋巴结中的淋巴细胞运输与自身免疫诱导之间存在机械联系。

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