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在肝脏再生过程中细胞周期进程中周期蛋白依赖性激酶(1和2)及细胞周期蛋白的表达与激活

Expression and activation of cdks (1 and 2) and cyclins in the cell cycle progression during liver regeneration.

作者信息

Loyer P, Glaise D, Cariou S, Baffet G, Meijer L, Guguen-Guillouzo C

机构信息

Institut National de la Santé et de la Recherche Médicale U49, Unité de Recherches Hépatologiques, Hôpital Pontchaillou, Rennes, France.

出版信息

J Biol Chem. 1994 Jan 28;269(4):2491-500.

PMID:8300575
Abstract

In normal adult liver, hepatocytes are arrested in G0, and they rapidly respond to a mass loss by a definite number of divisions. Thus, taking advantage of the in vivo regenerative capacity of the liver following partial hepatectomy, we have analyzed both expression and activation of p34cdc2 (= cdk1) and p33cdk2 through the cell cycle, particularly during the long lasting G1 phase and in the G1/S transition. While p33cdk2 is constantly expressed during the cell cycle, p34cdc2 is completely absent in resting hepatocytes and remains unexpressed for up to 20 h after partial hepatectomy, a time period corresponding to the G1 phase and G1/S transition, and then accumulates in the S, G2, and M phases. No histone H1 kinase activity is detected during the G1 phase, while two peaks of p34cdc2 kinase activity are observed during the S and M phases and only one peak of p33cdk2 kinase activity in the S phase. p34cdc2 forms complexes with both cyclins A and B while p33cdk2 is associated with cyclin A only. Surprisingly, cyclins E and D1 are present in resting liver and with modest variation throughout the cell cycle. Taken together, our data provide evidence that the pattern of G1-associated proteins in hepatocytes during liver regeneration is distinct from that described in other cell types.

摘要

在正常成年肝脏中,肝细胞停滞于G0期,并且它们会通过一定数量的分裂快速对质量损失做出反应。因此,利用部分肝切除术后肝脏的体内再生能力,我们分析了p34cdc2(= cdk1)和p33cdk2在整个细胞周期中的表达和激活情况,特别是在持续时间较长的G1期和G1/S转换期。虽然p33cdk2在细胞周期中持续表达,但p34cdc2在静止的肝细胞中完全不存在,并且在部分肝切除术后长达20小时内仍未表达,这一时间段对应于G1期和G1/S转换期,然后在S期、G2期和M期积累。在G1期未检测到组蛋白H1激酶活性,而在S期和M期观察到两个p34cdc2激酶活性峰,在S期仅观察到一个p33cdk2激酶活性峰。p34cdc2与细胞周期蛋白A和B都形成复合物,而p33cdk2仅与细胞周期蛋白A相关。令人惊讶的是,细胞周期蛋白E和D1存在于静止肝脏中,并且在整个细胞周期中变化不大。综上所述,我们的数据提供了证据,表明肝脏再生过程中肝细胞中与G1相关蛋白的模式与其他细胞类型中所描述的不同。

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