Growth-dependent inhibition of CCAAT enhancer-binding protein (C/EBP alpha) gene expression during hepatocyte proliferation in the regenerating liver and in culture.

D Mischoulon; B Rana; N L Bucher; S R Farmer

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Growth-dependent inhibition of CCAAT enhancer-binding protein (C/EBP alpha) gene expression during hepatocyte proliferation in the regenerating liver and in culture.

机译：CCAAT增强子结合蛋白（C / EBP alpha）基因表达在再生肝和培养物中肝细胞增殖过程中的生长依赖性抑制。

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As an approach to understanding physiological mechanisms that control the proliferation of highly differentiated cells, we are addressing whether certain hepatic transcription factors participate in mechanisms that control the growth of hepatocytes. We have focused on CCAAT enhancer-binding protein (C/EBP alpha), a transcription factor which is highly abundant in normal liver and is considered to regulate expression of many genes, including some involved in energy metabolism (S. L. McKnight, M. D. Lane, and S. Gluecksohn-Walsh. Genes Dev. 3:2021-2024, 1989). Using Northern (RNA) blot analysis, we have examined the expression of C/EBP alpha mRNA during liver regeneration and in primary cultures of hepatocytes. C/EBP alpha mRNA levels decrease 60 to 80% within 1 to 3 h after partial hepatectomy as the cells move from G0 to G1 and decrease further when cells progress into S phase. Run-on transcription analysis is in agreement with the Northern blot data, thus suggesting that C/EBP alpha is transcriptionally regulated in regenerating liver. C/EBP alpha mRNA expression also decreases dramatically during the growth of freshly isolated normal hepatocytes cultured under conventional conditions (on dried rat tail collagen; stimulated to proliferate by epidermal growth factor [EGF] and insulin). Cultures of hepatocytes on rat tail collagen in the presence or absence of EGF clearly show that within 3 h, EGF depresses C/EBP alpha mRNA expression and that this effect is substantially greater by 4 h. Inhibition of protein synthesis in the liver by cycloheximide or in cultured hepatocytes by puromycin or cycloheximide effectively blocks the down-regulation of C/EBP alpha gene expression, apparently by stabilizing the normal rapid turnover of the C/EBP alpha mRNA (half-life of <2 h). This drop in C/EBP alpha gene expression in response to activation of hepatocyte growth is consistent with the proposal that C/EBP alpha has an antiproliferative role to play in highly differentiated cells (R. M. Umek, A. D. Friedman, and S. L. McKnight, Science 251: 288-292, 1991).

机译：作为了解控制高分化细胞增殖的生理机制的一种方法，我们正在研究某些肝转录因子是否参与控制肝细胞生长的机制。我们专注于CCAAT增强子结合蛋白（C / EBP alpha），这是一种在正常肝脏中高度丰富的转录因子，被认为可以调节许多基因的表达，包括一些参与能量代谢的基因（SL McKnight，MD Lane和S.Gluecksohn-Walsh.Genes Dev.3：2021-2024，1989）。使用Northern（RNA）印迹分析，我们已经检查了肝再生和肝细胞原代培养中C / EBPαmRNA的表达。随着细胞从G0移至G1，C / EBPαmRNA水平在部分肝切除术后1至3小时内降低60％至80％，并在细胞进入S期时进一步降低。连续转录分析与Northern blot数据一致，因此表明C / EBPα在再生肝中受转录调控。在常规条件下（在干燥的大鼠尾部胶原上;经表皮生长因子[EGF]和胰岛素刺激增殖）新鲜分离的正常肝细胞的生长过程中，C / EBPαmRNA表达也急剧下降。在有或没有EGF的情况下，大鼠尾部胶原上的肝细胞培养物清楚地表明，EGF在3小时内抑制C / EBPαmRNA表达，并且这种作用在4 h时明显增强。环己酰亚胺抑制肝脏中的蛋白质合成，嘌呤霉素或环己酰亚胺抑制培养的肝细胞中的蛋白质合成有效地阻止了C / EBPα基因表达的下调，这显然是通过稳定C / EBPαmRNA的正常快速周转（半衰期<2小时）。响应于肝细胞生长激活的C / EBP alpha基因表达的这种下降与C / EBP alpha在高分化细胞中具有抗增殖作用的建议相符（RM Umek，AD Friedman和SL McKnight，Science 251： 288-292，1991）。

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《Molecular and Cellular Biology》 |1992年第6期|共8页
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D Mischoulon; B Rana; N L Bucher; S R Farmer;
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中图分类细胞生物学;
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Growth-dependent inhibition of CCAAT enhancer-binding protein (C/EBP alpha) gene expression during hepatocyte proliferation in the regenerating liver and in culture.

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