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人唾液酸结合免疫球蛋白样凝集素-5:组织分布、新型异构体及唾液酸依赖性配体相互作用的结构域特异性

Human Siglec-5: tissue distribution, novel isoforms and domain specificities for sialic acid-dependent ligand interactions.

作者信息

Connolly Nicholas P, Jones Margaret, Watt Suzanne M

机构信息

National Blood Service, Stem Cell Laboratory, National Blood Service Oxford Centre, John Radcliffe Hospital, Oxford, UK.

出版信息

Br J Haematol. 2002 Oct;119(1):221-38. doi: 10.1046/j.1365-2141.2002.03808.x.

Abstract

Human Siglec-5 is a sialic acid binding immunoglobulin (Ig)-like lectin (Siglec), comprising one N-terminal IgV-SET domain followed by three IgC2-SET domains, and a cytoplasmic domain with ITIM and SAP motifs which regulate cell signalling. We report the differential distribution of hSiglec-5 on neutrophil and macrophage subsets in tissues using monoclonal antibodies, 1A5 and 2H8, which require the first IgC2-SET domain for binding. Interestingly, hSiglec-5 was especially prominent on macrophages in reactive lymph nodes. We have identified four isoforms of hSiglec-5 possessing three (hSiglec-5-3L and -3C) or four (hSiglec-5-4L and -4S) extracellular domains linked to long (hSiglec-5-3L and -4L) or short (hSiglec-5-4S) cytoplasmic tails or existing as a soluble isoform (hSiglec-5-3C). hSiglec-5-4L has the broadest tissue distribution, being detected in adult spleen, thymus, lymph node, peripheral blood leucocytes and bone marrow, and in fetal lung and liver. A soluble Fc chimaeric protein containing the hSiglec-5-4L extracellular domain binds in a sialic acid-dependent manner to glycophorin A on human erythrocytes and to alpha2-3- and alpha2-6-sialyllactose moieties. Domain deletion mutants of hSiglec-5(D1-4)-Fc reveal that the first three IgC2-SET domains are required for optimal binding, with adhesion being abolished if the first IgC2-SET domain is deleted. This indicates that each hSiglec-5 isoform will interact with sialic acid ligands and provides the first step towards defining structure-function relationships of hSiglec-5 isoforms.

摘要

人唾液酸结合免疫球蛋白(Ig)样凝集素(Siglec)-5由一个N端IgV-SET结构域、三个IgC2-SET结构域以及一个带有免疫受体酪氨酸抑制基序(ITIM)和Src同源结构域(SH2)结合蛋白(SAP)基序的胞质结构域组成,这些基序可调节细胞信号传导。我们使用单克隆抗体1A5和2H8报告了hSiglec-5在组织中中性粒细胞和巨噬细胞亚群上的差异分布,这两种抗体结合需要第一个IgC2-SET结构域。有趣的是,hSiglec-5在反应性淋巴结的巨噬细胞上尤为突出。我们已经鉴定出hSiglec-5的四种异构体,它们具有三个(hSiglec-5-3L和-3C)或四个(hSiglec-5-4L和-4S)细胞外结构域,与长(hSiglec-5-3L和-4L)或短(hSiglec-5-4S)的胞质尾巴相连,或者以可溶性异构体(hSiglec-5-3C)的形式存在。hSiglec-5-4L具有最广泛的组织分布,在成人脾脏、胸腺、淋巴结、外周血白细胞和骨髓以及胎儿肺和肝脏中均可检测到。一种含有hSiglec-5-4L细胞外结构域的可溶性Fc嵌合蛋白以唾液酸依赖的方式与人红细胞上的血型糖蛋白A以及α2-3-和α2-6-唾液酸乳糖部分结合。hSiglec-5(D1-4)-Fc的结构域缺失突变体表明,前三个IgC2-SET结构域是最佳结合所必需的,如果删除第一个IgC2-SET结构域,粘附作用将被消除。这表明每种hSiglec-5异构体都将与唾液酸配体相互作用,并为定义hSiglec-5异构体的结构-功能关系提供了第一步。

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