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仅当CD4 + T细胞表达E选择素和P选择素的配体时,它们才会迁移到发炎的皮肤中。

CD4+ T cells migrate into inflamed skin only if they express ligands for E- and P-selectin.

作者信息

Tietz W, Allemand Y, Borges E, von Laer D, Hallmann R, Vestweber D, Hamann A

机构信息

Department of Immunology, Medical Clinic, University Hospital Eppendorf, Hamburg, Germany.

出版信息

J Immunol. 1998 Jul 15;161(2):963-70.

PMID:9670976
Abstract

Previous data suggested a role of endothelial selectins in skin homing of lymphocytes. In the current study, we have analyzed the expression and functional role of E-and P-selectin ligands on CD4+ T cells induced in vivo upon skin sensitization, using soluble selectin-Ig chimera and blocking Abs. Only low numbers of CD4+ cells expressing significant levels of E- or P-selectin ligands were present in s.c. lymph nodes of untreated mice (0.5-1.5% and 2-4%, respectively). Induction of a delayed-type hypersensitivity reaction increased the percentage of E-selectin-binding CD4+ cells in the draining lymph nodes up to 6 to 9% and that of P-selectin-binding cells up to 14%. The majority of E- and P-selectin-binding cells displayed an activated phenotype as judged by the increase in IL-2R, CD71, or cell size. The populations of E- and P-selectin-binding cells were largely overlapping; all E-selectin-binding cells also bound to P-selectin, whereas only a subfraction of P-selectin-binding cells reacted with E-selectin. Both E- and P-selectin-binding CD4+ cells, isolated by FACS, efficiently migrated into inflamed, but not normal skin, whereas P- or E-selectin ligand-negative CD4+ T cells did not. Abs against one of the two endothelial selectins partially inhibited the entry of isolated, ligand-positive cells, whereas a combination of Abs against both selectins almost completely abrogated skin homing. These data indicate that the expression of functional ligands for E- and for P-selectin is essential for homing of CD4+ T cells into the inflamed skin.

摘要

先前的数据表明内皮选择素在淋巴细胞归巢至皮肤过程中发挥作用。在本研究中,我们使用可溶性选择素-Ig嵌合体和阻断性抗体,分析了皮肤致敏后体内诱导产生的CD4⁺ T细胞上E-选择素和P-选择素配体的表达及功能作用。在未处理小鼠的皮下淋巴结中,仅有少量表达高水平E-或P-选择素配体的CD4⁺细胞(分别为0.5 - 1.5%和2 - 4%)。迟发型超敏反应的诱导使引流淋巴结中与E-选择素结合的CD4⁺细胞百分比增加至6% - 9%,与P-选择素结合的细胞百分比增加至14%。根据IL-2R、CD71或细胞大小的增加判断,大多数与E-和P-选择素结合的细胞呈现活化表型。与E-和P-选择素结合的细胞群体在很大程度上重叠;所有与E-选择素结合的细胞也与P-选择素结合,而只有一部分与P-选择素结合的细胞与E-选择素反应。通过荧光激活细胞分选术分离的与E-和P-选择素结合的CD4⁺细胞均能有效地迁移至炎症皮肤,但不能迁移至正常皮肤,而P-或E-选择素配体阴性的CD4⁺ T细胞则不能。针对两种内皮选择素之一的抗体部分抑制了分离出的配体阳性细胞的进入,而针对两种选择素的抗体组合几乎完全消除了皮肤归巢。这些数据表明,E-选择素和P-选择素功能性配体的表达对于CD4⁺ T细胞归巢至炎症皮肤至关重要。

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