首页> 外文期刊>The American Journal of Pathology >Topographic distribution of homing receptors on B and T cells in human gut-associated lymphoid tissue: Relation of L-selectin and integrin alpha4beta7 to naive and memory phenotypes
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Topographic distribution of homing receptors on B and T cells in human gut-associated lymphoid tissue: Relation of L-selectin and integrin alpha4beta7 to naive and memory phenotypes

机译:人类肠道相关淋巴组织中B和T细胞上归巢受体的地形分布:L-选择蛋白和整联蛋白alpha4beta7与幼稚和记忆表型的关系

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In mice, integrin alpha 4 beta 7 is the main receptor used by lymphocytes that home to the Peyer's patches, although L-selectin contributes to the initial interaction with high endothelial venules. Less is known about the expression and function of these adhesion molecules in humans. The distribution of L-selectin and alpha 4 beta 7 on various B- and T-cell subsets was examined in human Peyer's patches (n = 8) and appendix (n = 4), collectively called gut-associated lymphoid tissue. Multicolor immunophenotyping was performed on cryosections, and dispersed cells were examined by flow cytometry. In cryosections, CD45RA+ T cells around and within interfollicular high endothelial venules, as well as surface (s)IgD+ B lymphocytes in the follicle mantles, often expressed abundant L-selectin but only intermediate levels of alpha 4 beta 7. CD45RO+ T cells and sIgD- B cells expressed higher levels of alpha 4 beta 7 and were often located near putative efferent lymphatics; only a small fraction ( 20%) of such memory cells expressed L-selectin. By flow cytometry, considerably more T than B lymphocytes co-expressed L-selectin and alpha 4 beta 7 (40% versus 25% and 67% versus 39%, respectively). In samples with many L-selectin+ cells ( 30%), more of these lymphocytes co-expressed alpha 4 beta 7 than in samples with few L-selectin+ cells. Because L-selectin and alpha 4 beta 7 were co-expressed on lymphocytes located near high endothelial venules, and because such co-expression was relatively common when many L-selectin+ cells were present, both of these molecules might participate in homing to human gut-associated lymphoid tissue. Such homing is probably most pronounced for T lymphocytes that were found to express L-selectin and alpha 4 beta 7 more often than B lymphocytes. The selective and relatively high expression of alpha 4 beta 7 on memory cells located near efferent lymphatics indicated a different migratory capacity; after exit from gut-associated lymphoid tissue, such stimulated cells might home mainly to mucosal effector sites.
机译:在小鼠中,整联蛋白α4 beta 7是淋巴集结所在的淋巴细胞使用的主要受体,尽管L-选择蛋白有助于与高内皮微静脉的初始相互作用。这些黏附分子在人类中的表达和功能知之甚少。在人Peyer斑块(n = 8)和阑尾(n = 4)(统称为肠道相关淋巴组织)中检查了L-选择蛋白和alpha 4 beta 7在各种B细胞和T细胞亚群中的分布。在冷冻切片上进行多色免疫表型分析,并通过流式细胞仪检查分散的细胞。在冰冻切片中,小泡间高内皮小静脉周围和之内的CD45RA + T细胞以及滤泡套中的表面IgD + B淋巴细胞通常表达丰富的L-选择素,但仅中等水平的α4 beta7。CD45RO + T细胞和sIgD -B细胞表达较高水平的alpha 4 beta 7,并且通常位于假定的传出淋巴管附近;这种存储单元中只有一小部分(20%)表达L-选择蛋白。通过流式细胞术,共表达L-选择蛋白和α4beta 7的T细胞比B淋巴细胞多得多(分别为40%对25%和67%对39%)。在具有许多L-选择素+细胞的样品中(30%),与具有少量L-选择素+细胞的样品相比,更多的这些淋巴细胞共表达了alpha 4 beta 7。因为L-选择蛋白和alpha 4 beta 7在高内皮小静脉附近的淋巴细胞上共表达,并且因为当存在许多L-选择蛋白+细胞时这种共表达相对普遍,所以这两种分子都可能参与归巢至人类肠道-相关的淋巴组织。这种归巢对于发现比B淋巴细胞更频繁表达L-选择蛋白和alpha 4 beta 7的T淋巴细胞可能最为明显。 α4beta 7在传出淋巴管附近的记忆细胞上的选择性表达和相对较高的表达表明其迁移能力不同。从肠道相关的淋巴组织退出后,这种刺激的细胞可能主要归巢于粘膜效应位点。

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