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GRP78 positively regulates estrogen-stimulated cell growth mediated by ER-alpha 36 in gastric cancer cells

机译:GRP78积极地调节雌激素刺激的细胞生长,胃癌细胞中的ER-α36介导

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摘要

Estrogen receptor (ER)-alpha 36, a novel isoform of ER, primarily mediates non-classical estrogen signaling. It has been reported that ER-alpha 36-mediated growth stimulating signals are involved in the malignancy of gastric tumor cells. However, the mechanism underlying the regulation of ER-alpha 36 function in development of gastric cancer remains to be elucidated. The present study investigated the role of 78 kDa glucose-regulated protein (GRP78) in the regulation of ER-alpha 36 expression and signaling during the growth of gastric tumor cells. It was demonstrated that GRP78 expression was detectable in gastric cancer tumor tissues, and was positively-correlated with tumor stage, lymphatic metastasis and ER-alpha 36 expression (P<0.05). An increased growth rate, and increased expression of ER-alpha 36 and the cell cycle regulator cyclin D1 was detected in cells with GRP78 overexpression (SGC-High78 cells). SGC-High78 cells are more sensitive to estrogen compared with SGC-Control cells. Therefore, the results of the present study demonstrated that GRP78 positively regulated ER-alpha 36 expression and signaling with cell growth in gastric cancer, which is involved in gastric carcinogenesis.
机译:雌激素受体(ER)-α36,ER的新型同种型,主要是介导非经典雌激素信号。据报道,ER-α36介导的生长刺激信号参与胃肿瘤细胞的恶性程度。然而,待阐明ER-α36功能在胃癌遗体癌症的发展的调节基础的机制。本研究胃肿瘤细胞的生长期间调查了ER-α36表达和信令的第78 kDa的葡萄糖调节蛋白(GRP78)的作用。已经证实,GRP78的表达在胃癌肿瘤组织可检测的,并且与肿瘤分期,淋巴转移和ER-α36表达(P <0.05)中的溶液正相关。增加的生长速率,和ER-α36的表达增加,细胞周期调节蛋白D1在细胞中检测到与表达GRP78(SGC-High78细胞)。 SGC-High78细胞与SGC-对照细胞相比,雌激素更敏感。因此,本研究的结果表明,GRP78阳性调节ER-α36表达,并与胃癌,其参与胃癌细胞生长信号传导。

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