Onrust S V, Hartl P M, Rosen S D, Hanahan D
Department of Anatomy, University of California, San Francisco 94143, USA.
J Clin Invest. 1996 Jan 1;97(1):54-64. doi: 10.1172/JCI118406.
Immune surveillance depends on lymphocyte access to tissue. Lymphocytes emigrate from blood when adhesion receptors such as L-selectin and the alpha 4 beta 7 integrin on these cells bind to ligands expressed on venular endothelium. Among transgenic mouse lines expressing an oncoprotein (Tag) in islet beta cells, some recognize Tag as nonself. In these mice, Tag expression elicits both beta cell hyperplasia with subsequent progression to tumors and lymphocytic infiltration. Endothelial ligands for L-selectin and alpha 4 beta 7 were upregulated in infiltrated islets in these transgenic mice. These ligands were not expressed in tumors, which were devoid of lymphocytic infiltration. In contrast, the adhesion molecules PECAM-1, ICAM-1, and VCAM-1 were expressed on endothelium in both noninfiltrated tumors and infiltrated islets. Thus, upregulation of expression of endothelial ligands for L-selectin and alpha 4 beta 7 may contribute to autoimmune infiltration. Repression of expression of these same ligands may be involved in the failure of tumor immunity.
免疫监视依赖于淋巴细胞进入组织。当这些细胞上的黏附受体如L-选择素和α4β7整合素与小静脉内皮细胞上表达的配体结合时,淋巴细胞从血液中移出。在胰岛β细胞中表达癌蛋白(Tag)的转基因小鼠品系中,一些小鼠将Tag识别为非自身物质。在这些小鼠中,Tag的表达引发β细胞增生,随后发展为肿瘤以及淋巴细胞浸润。在这些转基因小鼠的浸润胰岛中,L-选择素和α4β7的内皮配体上调。这些配体在无淋巴细胞浸润的肿瘤中不表达。相反,黏附分子PECAM-1、ICAM-1和VCAM-1在未浸润的肿瘤和浸润的胰岛的内皮细胞上均有表达。因此,L-选择素和α4β7的内皮配体表达上调可能有助于自身免疫浸润。这些相同配体的表达受抑可能与肿瘤免疫失败有关。
