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淋巴细胞迁移的器官特异性:通过淋巴细胞与高内皮微静脉上的器官特异性决定簇的高度选择性相互作用介导。

Organ specificity of lymphocyte migration: mediation by highly selective lymphocyte interaction with organ-specific determinants on high endothelial venules.

作者信息

Butcher E C, Scollay R G, Weissman I L

出版信息

Eur J Immunol. 1980 Jul;10(7):556-61. doi: 10.1002/eji.1830100713.

Abstract

Evidence is presented that the organ specificity of lymphocyte migration is determined by selective interaction of lymphocytes with specialized endothelial cells. Mouse Peyer's patch and lymph node lymphocytes bind preferentially to high endothelial venules (HEV) in frozen sections of Peyer's patches and peripheral nodes, respectively, and this in vitro binding preference accurately predicts their differential segregation in vivo 30 min after i.v. injection. Both in vivo and in vitro, about 1.4 times as many as many Peyer's patch as lymph node lymphocytes bind HEV in Peyer's patches, and, conversely, twice as many lymph node cells interact with HEV in nonmesenteric lymph nodes. Even greater specificity is shown by certain homogeneous lymphocyte populations, i.e. thymic lymphomas. Some lymphomas bind with remarkable selectivity to HEV in Peyer's patches, and others interact almost exclusively with those in lymph nodes indicating that the mechanisms mediating selective recognition of HEV are capable of nearly absolute discrimination. Mesenteric node HEV are unique in that they allow both Peyer's patch- and lymph node-specific cells to bind. It is proposed that lymphocyte surface receptors specific for organ-restricted endothelial cell determinants mediate the antigen-independent organ specificity of lymphocyte migration. According to this model, there are at least 2 sets of complementary lymphocyte and endothelial cell receptors, one mediating lymphocyte-HEV adherence in Peyer's patches, the other in lymph nodes.

摘要

有证据表明,淋巴细胞迁移的器官特异性是由淋巴细胞与特殊内皮细胞的选择性相互作用所决定的。小鼠派伊尔结和淋巴结淋巴细胞分别优先与派伊尔结和外周淋巴结冰冻切片中的高内皮微静脉(HEV)结合,并且这种体外结合偏好准确地预测了静脉注射30分钟后它们在体内的差异分布。在体内和体外,派伊尔结淋巴细胞与派伊尔结中HEV结合的数量大约是淋巴结淋巴细胞的1.4倍,相反,淋巴结细胞与非肠系膜淋巴结中HEV相互作用的数量是派伊尔结淋巴细胞的两倍。某些同质淋巴细胞群体,即胸腺淋巴瘤,表现出更高的特异性。一些淋巴瘤对派伊尔结中的HEV具有显著的选择性结合,而另一些则几乎只与淋巴结中的HEV相互作用,这表明介导HEV选择性识别的机制能够进行近乎绝对的区分。肠系膜淋巴结HEV的独特之处在于它们允许派伊尔结特异性细胞和淋巴结特异性细胞都与之结合。有人提出,针对器官限制性内皮细胞决定簇的淋巴细胞表面受体介导了淋巴细胞迁移的抗原非依赖性器官特异性。根据这个模型,至少有两组互补的淋巴细胞和内皮细胞受体,一组介导派伊尔结中淋巴细胞与HEV的黏附,另一组介导淋巴结中的黏附。

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