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首页> 外文期刊>Oncogene >DLC-1 gene inhibits human breast cancer cell growth and in vivo tumorigenicity
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DLC-1 gene inhibits human breast cancer cell growth and in vivo tumorigenicity

机译:DLC-1基因抑制人乳腺癌细胞的生长和体内致瘤性

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摘要

The human DLC-1 (deleted in liver cancer 1) gene was cloned from a primary human hepatocellular carcinoma (HCC) and mapped to the chromosome 8p21–22 region frequently deleted in common human cancers and suspected to harbor tumor suppressor genes. DLC-1 was found to be deleted or downregulated in a significant number of HCCs. We expanded our investigations to other cancers with recurrent deletions of 8p22, and in this study examined alterations of DLC-1 in primary human breast tumors, human breast, colon, and prostate tumor cell lines. Genomic deletion of DLC-1 was observed in 40% of primary breast tumors, whereas reduced or undetectable levels of DLC-1 mRNA were seen in 70% of breast, 70% of colon, and 50% of prostate tumor cell lines To see whether DLC-1 expression affects cell growth and tumorigenicity, two breast carcinoma cell lines lacking the expression of endogenous gene were transfected with the DLC-1 cDNA. In both cell lines, DLC-1 transfection caused significant growth inhibition and reduction of colony formation. Furthermore, introduction of the DLC-1 cDNA abolished the in vivo tumorigenicity in nude mice, suggesting that the DLC-1 gene plays a role in breast cancer by acting as a bona fide tumor suppressor gene.
机译:从原发性人类肝细胞癌(HCC)中克隆了人类DLC-1(在肝癌1中缺失)基因,并将其定位到在常见人类癌症中经常缺失的8p21-22染色体区域,并怀疑具有肿瘤抑制基因。发现DLC-1在大量HCC中被删除或下调。我们将研究范围扩大到复发缺失8p22的其他癌症,并且在这项研究中研究了原发性人乳腺肿瘤,人乳腺,结肠和前列腺肿瘤细胞系中DLC-1的改变。在40%的原发性乳腺肿瘤中观察到DLC-1的基因组缺失,而在70%的乳腺,70%的结肠和50%的前列腺肿瘤细胞中DLC-1 mRNA的水平降低或无法检测为了观察DLC-1表达是否影响细胞生长和致瘤性,用DLC-1 cDNA转染了两种缺乏内源基因表达的乳腺癌细胞系。在这两种细胞系中,DLC-1转染均导致显着的生长抑制和集落形成的减少。此外,DLC-1 cDNA的导入消除了裸鼠体内的致瘤性,这表明DLC-1基因通过充当真正的肿瘤抑制基因在乳腺癌中发挥作用。

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