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A Critical Role for Dendritic Cells in the Formation of Lymphatic Vessels within Tertiary Lymphoid Structures

机译:树突状细胞在三级淋巴结构内的淋巴管形成中的关键作用。

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Ectopic, or tertiary, lymphoid aggregates often form in chronically inflamed areas. Lymphatic vessels, as well as high endothelial venules, form within these lymphoid aggregates, but the mechanisms underlying their development are poorly understood. Overexpression of the chemokine CCL21 in the thyroid of transgenic mice leads to formation of lymphoid aggregates containing topologically segregated T and B lymphocytes, dendritic cells (DCs), and specialized vasculature, including Lyve-1+/Prox-1+ lymphatic vessels. In this article, we show that adoptive transfer of mature CD4+ T cells into animals expressing CCL21 in a RAG-deficient background promotes the influx of host NK cells and DCs into the thyroid and the formation of new lymphatic vessels within 10 d. This process is dependent on the expression of lymphotoxin ligands by host cells, but not by the transferred CD4+ T cells. Ablation of host DCs, but not NK cells, reduces the formation of new lymphatic vessels in the thyroid. Taken together, these data suggest a critical role for CD11c+ DCs in the induction of lymphangiogenesis in tertiary lymphoid structures.
机译:异位或第三级淋巴样聚集物经常在慢性发炎区域形成。在这些淋巴样聚集物中形成了淋巴管以及高内皮小静脉,但对其发展的机制却知之甚少。转基因小鼠甲状腺中趋化因子CCL21的过表达导致形成淋巴样聚集体,其中包含拓扑分离的T和B淋巴细胞,树突状细胞(DC)和专门的脉管系统,包括Lyve-1 + / Prox-1 +淋巴管。在本文中,我们表明,成熟的CD4 + T细胞通过过继转移进入在RAG缺陷型背景中表达CCL21的动物中可促进宿主NK细胞和DC流入甲状腺并在10 d内形成新的淋巴管。该过程取决于宿主细胞而不是转移的CD4 + T细胞表达淋巴毒素配体。消融宿主DC而不是NK细胞,可减少甲状腺中新的淋巴管的形成。综上所述,这些数据表明CD11c + DC在诱导三级淋巴结构淋巴管生成中起关键作用。

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