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首页> 外文期刊>Journal of Biochemistry, The >Effects of the biological clock gene Bmal1 on tumour growth and anti-cancer drug activity
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Effects of the biological clock gene Bmal1 on tumour growth and anti-cancer drug activity

机译:生物钟基因Bmal1对肿瘤生长和抗癌活性的影响

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摘要

The Bmal1 gene plays a key role in controlling circadian rhythms. To better understand how the Bmal1 gene affects tumour growth and the response to anti-cancer drugs, we examined the effect of knockdown of Bmal1 by RNAi both in vitro and in vivo. Down-regulation of Bmal1 gene expression accelerated cell proliferation in vitro and promoted tumour growth in mice. Suppressing Bmal1 expression in murine colon cancer cells (C26) and fibroblast cells (L929) decreased apoptosis induced by Etoposid, reduced the distribution of cells in the G2/M phases treated by Docetaxel and decreased DNA damage induced by Cisplatin. Loss of Bmal1 reduced the expression of per1, per2, per3, wee1 and p53. The expression of p21 and c-myc was also altered in certain cell lines. However, Bmal1 deficiency increased the protein levels of cdc2, cyclin B1, cyclin D1 and cyclin E. Wee1 and cyclin A expression was minimally altered. Thus, the circadian clock gene Bmal1 plays a role in regulating tumour cell apoptosis, cell-cycle progression and DNA damage response and in homoeostasis regulation. Down-regulation of Bmal1 accelerates the development of tumours and may influence the response to anti-cancer drugs.
机译:Bmal1基因在控制昼夜节律中起关键作用。为了更好地了解Bmal1基因如何影响肿瘤生长以及对抗癌药的反应,我们在体内外检查了RNAi敲除Bmal1的作用。 Bmal1基因表达的下调加速了体外细胞增殖,并促进了小鼠的肿瘤生长。抑制鼠结肠癌细胞(C26)和成纤维细胞(L929)中的Bmal1表达可减少依托泊西汀诱导的细胞凋亡,减少多西他赛处理的G2 / M期细胞的分布,并减少顺铂诱导的DNA损伤。 Bmal1的丢失降低了per1,per2,per3,wee1和p53的表达。在某些细胞系中,p21和c-myc的表达也发生了改变。但是,Bmal1缺乏症增加了cdc2,cyclin B1,cyclin D1和cyclin E的蛋白质水平。Wee1和cyclin A的表达变化很小。因此,昼夜节律时钟基因Bmal1在调节肿瘤细胞凋亡,细胞周期进程和DNA损伤反应以及稳态调节中发挥作用。 Bmal1的下调会加速肿瘤的发展,并可能影响对抗癌药物的反应。

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