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首页> 外文期刊>BMC Cancer >Modulation of SIRT3 expression through CDK4/6 enhances the anti-cancer effect of sorafenib in hepatocellular carcinoma cells
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Modulation of SIRT3 expression through CDK4/6 enhances the anti-cancer effect of sorafenib in hepatocellular carcinoma cells

机译:通过CDK4 / 6调节SIRT3表达,增强了索拉芬蛋白在肝细胞癌细胞中的抗癌作用

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Hepatocellular carcinoma (HCC) is the leading cause of cancer-related deaths worldwide. The only drug currently approved for clinical use in the treatment of advanced HCC is sorafenib. However, many patients with HCC show reduced sensitivity to sorafenib during treatment. SIRT3, a member of the mammalian sirtuin family, is a tumor suppressor in certain tumor types. However, only few studies have investigated the effects of SIRT3 on tumor prognosis and sorafenib sensitivity in patients with HCC. Here, we aimed to investigate the correlation between SIRT3 expression and glucose metabolism and proliferation in HCC and discover effective compounds that increase endogenous SIRT3 modulation effect of sorafenib. To determine the correlation between SIRT3 and glucose related proteins, immunostaining was performed with liver cancer tissue using various antibodies. To investigate whether the expression of SIRT3 in HCC is related to the resistance to sorafenib, we treated sorafenib after the modulation of SIRT3 levels in HCC cell lines (overexpression in Huh7, knockdown in HepG2). We also employed PD0332991 to modulate the SIRT3 expression in HCC cell and conducted functional assays. SIRT3 expression was downregulated in high glycolytic and proliferative HCC cells of human patients, xenograft model and HCC cell lines. Moreover, SIRT3 expression was downregulated after sorafenib treatment, resulting in reduced drug sensitivity in HCC cell lines. To enhance the anti-tumor effect of sorafenib, we employed PD0332991 (CDK4/6-Rb inhibitor) based on the correlation between SIRT3 and phosphorylated retinoblastoma protein in HCC. Notably, combined treatment with sorafenib and PD0332991 showed an enhancement of the anti-tumor effect in HCC cells. Our data suggest that the modulation of SIRT3 by CDK4/6 inhibition might be useful for HCC therapy together with sorafenib, which, unfortunately, has limited efficacy and whose use is often associated with drug resistance.
机译:肝细胞癌(HCC)是全世界癌症相关死亡的主要原因。目前批准用于治疗晚期HCC临床用途的唯一药物是索拉非尼。然而,许多HCC患者在治疗期间显示对索拉非尼的敏感性降低。 SIRT3是哺乳动物Sirtuin家族的成员,是某些肿瘤类型的肿瘤抑制因素。然而,只有很少的研究已经研究了SIRT3对HCC患者肿瘤预后和索拉非尼敏感性的影响。在此,我们旨在探讨HCC中SIRT3表达和葡萄糖代谢和增殖的相关性,并发现索拉芬蛋白增强内源性SIRT3调节效果的有效化合物。为了确定SIRT3和葡萄糖相关蛋白质之间的相关性,使用各种抗体用肝癌组织进行免疫染色。为了探讨HCC中SIRT3的表达是否与索拉非尼的抗性有关,我们在HCC细胞系中调节SIRT3水平后对Sorafenib进行了治疗(HUH7中的过表达,Hepg2敲低)。我们还使用PD0332991来调节HCC细胞中的SIRT3表达并进行功能测定。 SIRT3表达在人类患者,异种移植模型和HCC细胞系的高糖酵解和增殖HCC细胞中下调。此外,SIRT3表达在Sorafenib处理后下调,导致HCC细胞系中的药物敏感性降低。为了增强索拉非尼的抗肿瘤作用,基于HCC中SIRT3和磷酸化视网膜瘤蛋白的相关性基于PD0332991(CDK4 / 6-RB抑制剂)。值得注意的是,与索拉非尼和PD0332991的组合治疗表明HCC细胞中抗肿瘤作用的增强。我们的数据表明,CDK4 / 6抑制的SIRT3调节可能对HCC治疗与索拉非尼一起有用,这不幸的是,其效力有限,其用途通常与耐药性有关。

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