Progression through G1 and S phases of adult rat hepatocytes.

Progress in cell cycle research Pub Date : 1996-01-01 DOI:10.1007/978-1-4615-5873-6_4

P Loyer, G Ilyin, S Cariou, D Glaise, A Corlu, C Guguen-Guillouzo

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引用次数: 30

Abstract

Regenerating liver, hepatocyte primary cultures and differentiated hepatoma cell lines are widely used to study the proliferation/differentiation/apoptosis equilibrium in liver. In hepatocytes, priming factors (TNF alpha, IL6) target G0/G1 transition while growth factors (HGF, EGF, TGF alpha) control a mid-late G1 restriction point. A characteristic pattern of cdk/cyclin expression is observed in hepatocytes, presumably related to their ability to proliferate a limited number of times and to undergo a reversible differentiation. Interestingly, cell-cell interactions between hepatocytes and liver biliary cells in co-cultures, result in a cell cycle arrest in mid G1 of hepatocytes which are insensitive to mitogens. Apoptosis exists in hepatocytes but is still poorly documented. However, hepatoma cell lines stimulated by TGF beta undergo cell death in a p53-independent pathway. In conclusion, the interplay of growth and apoptosis regulators and cell-cell interactions control the proliferation/differentiation/apoptosis balance which is a specific feature of hepatocytes.

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成年大鼠肝细胞G1期和S期的进展。

再生肝、肝细胞原代培养和分化肝癌细胞系被广泛用于研究肝脏的增殖/分化/凋亡平衡。在肝细胞中，启动因子(TNF α、IL6)靶向G0/G1过渡，而生长因子(HGF、EGF、TGF α)控制G1中后期的限制点。在肝细胞中观察到cdk/cyclin表达的特征性模式，可能与它们增殖有限次数和经历可逆分化的能力有关。有趣的是，在共培养中，肝细胞和肝胆道细胞之间的细胞-细胞相互作用导致对丝裂原不敏感的肝细胞在G1期中期细胞周期阻滞。细胞凋亡存在于肝细胞中，但文献记载甚少。然而，TGF β刺激的肝癌细胞系通过p53不依赖的途径发生细胞死亡。总之，生长和凋亡调节因子的相互作用以及细胞间的相互作用控制着肝细胞的增殖/分化/凋亡平衡，这是肝细胞的一个特殊特征。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Progress in cell cycle research

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