首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >A second major native von Hippel–Lindau gene product initiated from an internal translation start site functions as a tumor suppressor
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A second major native von Hippel–Lindau gene product initiated from an internal translation start site functions as a tumor suppressor

机译:从内部翻译起始位点开始的第二种主要的天然von Hippel–Lindau基因主要产物起着抑癌作用

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摘要

The von Hippel–Lindau (VHL) tumor suppressor gene is inactivated in both sporadic and inherited clear cell renal carcinoma associated with VHL disease. We have identified two distinct native products of the human VHL gene, with apparent molecular masses of 24 and 18 kDa. The 18-kDa VHL protein was more abundant in nearly all cell lines examined. Reintroduction of the 18-kDa VHL gene product into renal carcinoma cells lacking wild-type VHL protein led to down-regulation of vascular endothelial growth factor (VEGF) mRNA and glucose transporter GLUT1 protein and suppressed tumor formation in nude mice. The 18-kDa VHL protein also demonstrated binding to elongins B and C. In an in vitro assay, the second in-frame AUG codon present in VHL mRNA was shown to be necessary and sufficient for production of the 18-kDa VHL protein, consistent with an internal translation mechanism. These data provide evidence for a second major VHL gene product, which contains the functional domains of the VHL gene. Moreover, these results indicate that internal translation initiation is an important mechanism for production of the major VHL protein.
机译:von Hippel–Lindau(VHL)肿瘤抑制基因在与VHL疾病相关的散发性和遗传性透明细胞肾癌中均失活。我们已经确定了人类VHL基因的两种不同的天然产物,其表观分子质量分别为24和18 kDa。在几乎所有检查的细胞系中,18 kDa VHL蛋白含量更高。将18 kDa VHL基因产物重新引入缺乏野生型VHL蛋白的肾癌细胞中导致血管内皮生长因子(VEGF)mRNA和葡萄糖转运蛋白GLUT1蛋白下调,并抑制了裸鼠的肿瘤形成。 18 kDa VHL蛋白还显示出与延伸蛋白B和C的结合。在体外测定中,显示出VHL mRNA中存在的第二个框内AUG密码子对于生产18 kDa VHL蛋白是必要且足够的,这是一致的。具有内部翻译机制。这些数据为第二种主要VHL基因产物提供了证据,该产物包含VHL基因的功能域。而且,这些结果表明内部翻译起始是产生主要VHL蛋白的重要机制。

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