首页> 外文期刊>Molecular Carcinogenesis >Wild-type APC regulates caveolin-1 expression in human colon adenocarcinoma cell lines via FOXO1a and C-myc.
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Wild-type APC regulates caveolin-1 expression in human colon adenocarcinoma cell lines via FOXO1a and C-myc.

机译:野生型APC通过FOXO1a和C-myc调节人结肠腺癌细胞系中Caveolin-1的表达。

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摘要

Genetic evidence suggests that caveolin-1, an essential component of membrane caveolae, acts as a tumor promoter in some, and a tumor suppressor in other cancers. The role of caveolin-1 in colon carcinogenesis is controversial. We report here, for the first time, that caveolin-1 is transcriptionally induced in colon cancer cells in response to conditional expression of a full length adenomatous polyposis coli (APC) gene. This induction of caveolin-1 by APC is mediated by both FOXO1a, a member of the Forkhead family of transcription factor, and c-myc. The FOXO1a protein, which is increased by wild-type APC expression, induces caveolin-1 promoter-reporter activity and binds directly to a FKHR consensus binding sequence in the caveolin-1 promoter. The c-myc protein, which is reduced in the presence of wild-type APC, acts to repress caveolin-1 expression by acting at non-E-box containing elements in the caveolin-1 promoter. These data predict that caveolin-1 protein expression would be decreased early in colonic carcinogenesis, which is associated with loss of wild-type APC. Our results would be consistent with the interpretation that caveolin-1 may have tumor suppressing functions during early stages of colon carcinogenesis.
机译:遗传证据表明,caveolin-1是膜小窝膜的重要组成部分,在某些癌症中起着肿瘤促进剂的作用,而在其他癌症中起着抑癌作用。 Caveolin-1在结肠癌发生中的作用是有争议的。我们在这里首次报道,响应于全长腺瘤性息肉病大肠杆菌(APC)基因的条件表达,caveolin-1在结肠癌细胞中被转录诱导。 APC对小窝蛋白1的诱导是由FOXO1a(即Forkhead转录因子家族的成员)和c-myc介导的。通过野生型APC表达增加的FOXO1a蛋白诱导小窝蛋白1启动子-报告子活性,并直接与小窝蛋白1启动子中的FKHR共有结合序列结合。在野生型APC存在下还原的c-myc蛋白可通过作用于Caveolin-1启动子中不含E-box的元件来抑制Caveolin-1的表达。这些数据预测,在结肠癌发生过程中,caveolin-1蛋白的表达会降低,这与野生型APC的丧失有关。我们的结果与以下解释是一致的:caveolin-1可能在结肠癌发生的早期阶段具有抑制肿瘤的功能。

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