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转化生长因子-β(TGF-β)在肝细胞中上调烟酰胺腺嘌呤二核苷酸磷酸(NADPH)氧化酶NOX4对其促凋亡活性是必需的。

Upregulation of the NADPH oxidase NOX4 by TGF-beta in hepatocytes is required for its pro-apoptotic activity.

作者信息

Carmona-Cuenca Irene, Roncero César, Sancho Patricia, Caja Laia, Fausto Nelson, Fernández Margarita, Fabregat Isabel

机构信息

Departamento de Bioquímica y Biología Molecular, Facultad de Farmacia, Universidad Complutense, 28040 Madrid, Spain.

出版信息

J Hepatol. 2008 Dec;49(6):965-76. doi: 10.1016/j.jhep.2008.07.021. Epub 2008 Sep 19.

DOI:10.1016/j.jhep.2008.07.021
PMID:18845355
Abstract

BACKGROUND/AIMS: The transforming growth factor-beta (TGF-beta) induces apoptosis in hepatocytes through an oxidative stress process. Here, we have analyzed the role of different NADPH oxidase isoforms in the intracellular signalling induced by TGF-beta in hepatocytes, to later explore whether this mechanism is altered in liver tumor cells.

METHODS

Primary cultures of rat and human hepatocytes, HepG2 and Hep3B cells were used in in vitro studies to analyze the TGF-beta response.

RESULTS

TGF-beta-induced apoptosis in rat hepatocytes does not require Rac-dependent NADPH oxidases. TGF-beta upregulates the Rac-independent Nox4, which correlates with its pro-apoptotic activity. Regulation of Nox4 occurs at the transcriptional level and is counteracted by intracellular survival signals. siRNA targeted knock-down of Nox4 attenuates NADPH oxidase activity, caspase activation and cell death in rat hepatocytes. NOX4 upregulation by TGF-beta is also observed in human hepatocytes, coincident with apoptosis. In human hepatocellular carcinoma (HCC) cell lines, NOX4 upregulation by TGF-beta is only observed in cells that are sensitive to its cytotoxic effect, such as Hep3B cells. siRNA targeted knock-down of NOX4 in these cells impairs TGF-beta-induced apoptosis.

CONCLUSIONS

Upregulation of NOX4 by TGF-beta is required for its pro-apoptotic activity in hepatocytes. Impairment of this TGF-beta-induced response might confer apoptosis resistance in HCC cells.

摘要

背景/目的:转化生长因子-β(TGF-β)通过氧化应激过程诱导肝细胞凋亡。在此,我们分析了不同NADPH氧化酶同工型在TGF-β诱导的肝细胞内信号传导中的作用,随后探讨该机制在肝肿瘤细胞中是否发生改变。

方法

大鼠和人肝细胞原代培养物、HepG2和Hep3B细胞用于体外研究以分析TGF-β反应。

结果

TGF-β诱导的大鼠肝细胞凋亡不需要Rac依赖性NADPH氧化酶。TGF-β上调不依赖Rac的Nox4,这与其促凋亡活性相关。Nox4的调节发生在转录水平,并被细胞内存活信号抵消。靶向敲低Nox4的siRNA可减弱大鼠肝细胞中的NADPH氧化酶活性、半胱天冬酶激活和细胞死亡。在人肝细胞中也观察到TGF-β上调NOX4,与凋亡一致。在人肝细胞癌(HCC)细胞系中,仅在对其细胞毒性作用敏感的细胞(如Hep3B细胞)中观察到TGF-β上调NOX4。在这些细胞中靶向敲低NOX4的siRNA会损害TGF-β诱导的凋亡。

结论

TGF-β上调NOX4是其在肝细胞中促凋亡活性所必需的。这种TGF-β诱导反应的受损可能赋予HCC细胞凋亡抗性。

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