G Anastassiou, S Duensing, G Steinhoff, H Kirchner, A Ganser, J Atzpodien
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引用次数: 12
摘要
我们使用针对VLA整合素亚基(VLA-1至VLA-6)和CD51的单克隆抗体,通过免疫组化研究了23例肾细胞癌和2例正常肾组织。我们研究的所有整合素,除了VLA-4(普遍阴性),在肿瘤中以不同的模式分布。我们发现vas -2的表达与组织部位相关;原代肿瘤细胞不表达vla2整合素,而来自转移组织的肿瘤细胞表达vla2整合素(P < 0.009)。此外,vegf -3和vegf -5的表达与肿瘤分级相关;这两种整合素在G1肿瘤中均未检测到,但在G2和G3肿瘤中广泛表达(vla3, p < .000;vla5, p < .005)。我们的研究结果表明,vas -2整合素参与了RCC的转移,并且与正常或高分化的肿瘤细胞相比,低分化的肿瘤细胞具有不同的整合素表型。
In vivo distribution of integrins in renal cell carcinoma: integrin-phenotype alteration in different degrees of tumor differentiation and VLA-2 involvement in tumor metastasis.
We studied 23 renal cell carcinomas and two normal kidney tissues by immunohistochemistry using monoclonal antibodies against subunits of the VLA integrins (VLA-1 to VLA-6) and CD51. All integrins investigated in our study, except VLA-4 (ubiquitous negative), were distributed in different patterns in tumors assayed. We found a correlation between VLA-2 expression and site of tissue; primary tumor cells expressed no VLA-2 integrin, whereas tumor cells from metastatic tissues exhibited VLA-2 positivity (P < .009). Additionally, the expression of VLA-3 and VLA-5 correlated with tumor grading; both integrins were undetectable in G1 tumors but widely expressed in G2 and G3 tumors (VLA-3, p < .000; VLA-5, p < .005). Our results suggest that VLA-2 integrin is involved in metastasis of RCC and that poorly differentiated tumor cells have a different integrin phenotype when compared to normal or highly differentiated tumor cells.