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一种归巢受体-IgG嵌合体作为淋巴结高内皮微静脉黏附配体的探针。

A homing receptor-IgG chimera as a probe for adhesive ligands of lymph node high endothelial venules.

作者信息

Watson S R, Imai Y, Fennie C, Geoffroy J S, Rosen S D, Lasky L A

机构信息

Department of Immunobiology, Genentech, Inc., South San Francisco, California 94080.

出版信息

J Cell Biol. 1990 Jun;110(6):2221-9. doi: 10.1083/jcb.110.6.2221.

Abstract

The binding of lymphocytes to high endothelial venules (HEV) within peripheral lymph nodes (pln) is thought to be mediated by a lectinlike adhesion molecule termed the pln homing receptor (pln HR). The cloning and sequencing of cDNAs encoding both murine and human pln HR revealed that these adhesion molecules contain protein motifs that are homologous to C-type or calcium dependent lectin domains as well as to epidermal growth factor (egf) and complement-regulatory protein domains. We have produced a novel, antibody-like form of the murine HR by joining the extracellular region of the receptor to a human IgG heavy chain. This antibody-like molecule is capable of recognizing carbohydrates, blocking the binding of lymphocytes to pln HEV, and serving as a histochemical reagent for the staining of pln HEV. This murine HR-IgG chimera should prove useful in analyzing the distribution of the HR ligand(s) in normal as well as in inflammatory states.

摘要

淋巴细胞与外周淋巴结(pln)内的高内皮微静脉(HEV)的结合被认为是由一种称为pln归巢受体(pln HR)的凝集素样粘附分子介导的。编码小鼠和人pln HR的cDNA的克隆和测序表明,这些粘附分子含有与C型或钙依赖性凝集素结构域以及表皮生长因子(EGF)和补体调节蛋白结构域同源的蛋白质基序。我们通过将受体的细胞外区域与人IgG重链连接,产生了一种新型的、抗体样形式的小鼠HR。这种抗体样分子能够识别碳水化合物,阻断淋巴细胞与pln HEV的结合,并作为pln HEV染色的组织化学试剂。这种小鼠HR-IgG嵌合体在分析正常和炎症状态下HR配体的分布方面应该会被证明是有用的。

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