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淋巴细胞归巢受体的内皮配体上唾液酸的需求。

Requirement for sialic acid on the endothelial ligand of a lymphocyte homing receptor.

作者信息

True D D, Singer M S, Lasky L A, Rosen S D

机构信息

Department of Anatomy, University of California, San Francisco 94143-0452.

出版信息

J Cell Biol. 1990 Dec;111(6 Pt 1):2757-64. doi: 10.1083/jcb.111.6.2757.

Abstract

The entry of blood-borne lymphocytes into most secondary lymphoid organs is initiated by a highly specific adhesive interaction with the specialized cuboidal endothelial cells of high endothelial venules (HEV). The adhesive receptors on lymphocytes that dictate interactions with HEV in different lymphoid organs are called homing receptors, signifying their critical role in controlling organ-selective lymphocyte migration. Considerable work has established that the mouse peripheral lymph node homing receptor (pnHR), defined by the mAb MEL-14, functions as a lectin-like adhesive protein. We have previously shown that sialidase treatment of peripheral lymph node (PN) HEV abrogates lymphocyte attachment to the HEV both in vivo and in vitro. We extend this evidence by demonstrating that Limax agglutinin (LA), a sialic acid-specific lectin, when reacted with HEV exposed in cryostat-cut tissue sections, blocks lymphocyte attachment to PN HEV and, unexpectedly, to the HEV of Peyer's patches (PP) as well. Using a recombinant form of the pnHR as a histochemical probe for its cognate adhesive site (HEV-ligand) on PN HEV, we demonstrate that both sialidase and Limax agglutinin functionally inactive this ligand. It is concluded that the requirement for sialic acid is at the level of the pnHR interaction with its HEV ligand. A distinct sialyloligosaccharide may encode the recognition determinant of a PP HEV ligand.

摘要

血源性淋巴细胞进入大多数二级淋巴器官是由与高内皮微静脉(HEV)的特殊立方内皮细胞发生高度特异性黏附相互作用启动的。淋巴细胞上决定其与不同淋巴器官中HEV相互作用的黏附受体被称为归巢受体,这表明它们在控制器官选择性淋巴细胞迁移中起关键作用。大量研究已证实,由单克隆抗体MEL-14定义的小鼠外周淋巴结归巢受体(pnHR)作为一种凝集素样黏附蛋白发挥作用。我们之前已表明,对外周淋巴结(PN)HEV进行唾液酸酶处理可在体内和体外消除淋巴细胞与HEV的附着。我们通过证明一种唾液酸特异性凝集素——雨蛙凝集素(LA),在与冷冻切片组织中暴露的HEV反应时,可阻断淋巴细胞与PN HEV以及出人意料地与派尔集合淋巴结(PP)的HEV的附着,从而扩展了这一证据。使用重组形式的pnHR作为其在PN HEV上同源黏附位点(HEV配体)的组织化学探针,我们证明唾液酸酶和雨蛙凝集素均可使该配体失活。结论是,对唾液酸的需求处于pnHR与其HEV配体相互作用的水平。一种独特的唾液酸化寡糖可能编码PP HEV配体的识别决定簇。

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Chemistry, metabolism, and biological functions of sialic acids.唾液酸的化学、代谢及生物学功能
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