肿瘤细胞表面α 4 β 1整合素介导血管内皮粘附:与INCAM-110/VCAM-1 n端结构域相互作用的证明

D B Taichman, M I Cybulsky, I Djaffar, B M Longenecker, J Teixidó, G E Rice, A Aruffo, M P Bevilacqua
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引用次数: 114

摘要

血液转移涉及血源性肿瘤细胞与血管壁之间的黏附相互作用。通过体外实验,人类黑色素瘤、骨肉瘤和肾癌(但不包括结肠癌)细胞系的粘附被证明涉及细胞因子诱导的内皮细胞表面蛋白诱导细胞粘附分子110 (INCAM-110)和α 4 β 1整合素,这些分子通常参与内皮-白细胞相互作用。肿瘤坏死因子(Tumor necrosis factor, TNF)激活内皮细胞后,肿瘤对人内皮细胞单层的粘附性增加1.9 ~ 8.2倍,抗incam -110单克隆抗体(mAb) E1/6抑制肿瘤的粘附性。这些肿瘤细胞都表达粘附分子的β 1整合素家族成员,α 4和β 1整合素亚基的抗体抑制肿瘤内皮粘附(48-87%的抑制)。一个包含血管细胞粘附分子1 (VCAM-1)的三个n端igg样结构域的cDNA编码了一个被抗incam -110 mAb E1/6识别的蛋白,当被捕获到塑料上时,通过α 4整合素依赖机制支持黑色素瘤细胞粘附。与mAb E1/6相比,第二个抗INCAM-110 mAb Hu8/4既不抑制对活化内皮的粘附,也不结合INCAM-110/VCAM-1的前三个ig样结构域。这些数据表明,几种人类肿瘤对活化内皮细胞的粘附是由α 4 β 1整合素和内皮细胞INCAM-110/VCAM-1的n端ig样结构域的相互作用介导的。肿瘤获得α 4整合素亚基和内皮细胞表达INCAM-110可能影响转移的频率和分布。
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Tumor cell surface alpha 4 beta 1 integrin mediates adhesion to vascular endothelium: demonstration of an interaction with the N-terminal domains of INCAM-110/VCAM-1.

Hematogenous metastasis involves adhesive interactions between blood-borne tumor cells and the vessel wall. By the use of in vitro assays, the adhesion of human melanoma, osteosarcoma, and kidney carcinoma (but not colon carcinoma) cell lines was shown to involve the cytokine-inducible endothelial cell surface protein inducible cell adhesion molecule 110 (INCAM-110) and the alpha 4 beta 1 integrin, molecules normally involved in endothelial-leukocyte interactions. Tumor adhesion to human endothelial cell monolayers was increased 1.9- to 8.2-fold by endothelial activation with the cytokine tumor necrosis factor (TNF) and inhibited by the anti-INCAM-110 monoclonal antibody (mAb) E1/6. Each of these tumor cells expressed members of the beta 1 integrin family of adhesion molecules, and antibodies to the alpha 4 and beta 1 integrin subunits inhibited tumor-endothelial adhesion (48-87% inhibition). A cDNA encompassing the three N-terminal Ig-like domains of vascular cell adhesion molecule 1 (VCAM-1) encoded a protein recognized by the anti-INCAM-110 mAb E1/6 and, when captured onto plastic, supported melanoma cell adhesion by an alpha 4 integrin-dependent mechanism. In contrast to mAb E1/6, a second anti-INCAM-110 mAb Hu8/4 neither inhibited adhesion to activated endothelium nor bound the first three Ig-like domains of INCAM-110/VCAM-1. These data indicate that the adherence of several human tumors to activated endothelium is mediated by an interaction of alpha 4 beta 1 integrin and the N-terminal Ig-like domains of endothelial INCAM-110/VCAM-1. Tumor acquisition of the alpha 4 integrin subunit and endothelial expression of INCAM-110 may affect the frequency and distribution of metastasis.

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