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首页> 外文期刊>Oncogene >LIM-class homeobox gene Lim1, a novel oncogene in human renal cell carcinoma
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LIM-class homeobox gene Lim1, a novel oncogene in human renal cell carcinoma

机译:LIM类同源异型盒基因Lim1,人类肾细胞癌中的新型致癌基因

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Human clear cell renal cell carcinoma (CCC) remains resistant to therapies. The transcription factor LIM-class homeobox gene Lim1 is required for normal organogenesis, including nephrogenesis, by regulating cell movements, differentiation and growth. Its expression is controlled partly by the sonic hedgehog-Gli signaling pathway, which we have recently shown to be reactivated in human CCC. So far, no study has assessed whether Lim1 may be associated with tumorigenesis. Using a panel of human CCC cell lines expressing or not the von Hippel-Lindau tumor suppressor gene and 44 tumorormal tissues pairs, we found that Lim1 is constitutively and exclusively reexpressed in tumors. Through Lim1 silencing or overexpressing, we show that Lim1 is a growth and survival factor in human CCC, at least through the activation of oncogenic pathways including the phosphoinositide kinase-3/Akt and nuclear factor-kappaB pathways. More importantly, in nude mice bearing human CCC tumors, Lim1 silencing abolished tumor growth through the same mechanism as in vitro . In Lim1-depleted cells and tumors, cell movements were substantially impaired because of the inhibition of expression of various proteins involved in metastatic spread, such as paxillin or tenascin-C. These findings establish that the developmental marker Lim1 acts as an oncogene in cancer cells and targeting Lim1 may constitute an innovative therapeutic intervention in human CCC.
机译:人类透明细胞肾细胞癌(CCC)仍然对疗法有抵抗力。转录因子LIM类同源盒基因Lim1是正常器官发生(包括肾发生)所必需的,它通过调节细胞运动,分化和生长来实现。它的表达部分受声音刺猬-Gli信号通路的控制,我们最近证明该通路在人CCC中可以被重新激活。到目前为止,尚无研究评估Lim1是否可能与肿瘤发生有关。使用一组表达或不表达von Hippel-Lindau抑癌基因的人类CCC细胞系和44个肿瘤/正常组织对,我们发现Lim1在肿瘤中组成性且专门重新表达。通过Lim1沉默或过表达,我们表明Lim1是人类CCC中的生长和生存因子,至少通过激活致癌途径(包括磷酸肌醇激酶-3 / Akt和核因子-κB途径)来实现。更重要的是,在携带人CCC肿瘤的裸鼠中,Lim1沉默通过与体外相同的机制消除了肿瘤的生长。在消耗Lim1的细胞和肿瘤中,由于抑制了与转移扩散有关的各种蛋白质(如Paxillin或Tenascin-C)的表达,因此大大削弱了细胞运动。这些发现证实,发育标记Lim1在癌细胞中起癌基因的作用,靶向Lim1可能构成对人CCC的创新治疗干预。

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