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Reduced Levels of Transforming Growth Factor‐beta Type I Receptor in Human Gastric Carcinomas

机译:降低人类胃癌中转化生长因子-βI型受体的水平

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摘要

The expressions of transforming growth factor beta (TGF‐β) and its receptor and TGF‐β inhibitory element (TIE)‐binding protein were examined on human gastric carcinomas by Northern blot hybridization, immunohistochemistry, affinity labeling and gel retardation analysis. TGF‐β mRNA was expressed in tumor and normal tissues at various levels. Immunohistochemically, TGF‐β expression was confirmed to be present within tumor cells. Out of the 17 human gastric carcinoma tissues, 14 (82%) showed a reduction in the level of type I receptor (65 kDa) for TGF‐β when compared to corresponding normal mucosas. Interestingly, in seven of the 14 tumors the level of TIE‐binding protein in the tumor tissue was lower than that in normal mucosa. Human gastric carcinoma cell line TMK‐1, whose growth was inhibited by TGF‐β, had only type I receptor for TGF‐β and showed a high level of TIE‐binding protein. Conversely, MKN‐1, a TGF‐β ‐resistant cell line, exhibited an extremely low level of TGF‐β receptor and had no TIE‐binding protein. These results overall indicate that although human gastric carcinoma cells produced TGF‐β, they showed a reduction in TGF‐β type I receptor and a low level of TIE‐binding protein, resulting in escape from growth inhibition by TGF‐β.
机译:通过Northern印迹杂交,免疫组织化学,亲和标记和凝胶阻滞分析,检测了人胃癌中转化生长因子β(TGF-β)及其受体和TGF-β抑制元件(TIE)结合蛋白的表达。 TGF-βmRNA在肿瘤和正常组织中以不同水平表达。免疫组织化学证实,TGF-β表达存在于肿瘤细胞中。与相应的正常粘膜相比,在17种人胃癌组织中,有14种(82%)显示出TGF-β的I型受体水平(65 kDa)降低。有趣的是,在14种肿瘤中的7种中,肿瘤组织中TIE结合蛋白的水平低于正常黏膜。 TGF-β抑制了其生长的人胃癌细胞系TMK-1,仅具有TGF-β的I型受体,并显示出高水平的TIE结合蛋白。相反,MKN-1是一种TGF-β耐药细胞系,其TGF-β受体水平极低,并且没有TIE结合蛋白。这些结果总体上表明,尽管人类胃癌细胞产生了TGF-β,但它们显示出I型TGF-β受体的减少和TIE结合蛋白的水平较低,从而导致逃避了TGF-β的生长抑制。

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