原代培养鸡肝细胞短期缺氧诱导DNA合成的潜在机制：Ca(2+)/PKC/MAPKs与PI3K/Akt/mTOR之间的相关性

A potential mechanism for short time exposure to hypoxia-induced DNA synthesis in primary cultured chicken hepatocytes: Correlation between Ca(2+)/PKC/MAPKs and PI3K/Akt/mTOR.

作者信息

Lee Sang Hun, Lee Min Young, Lee Jang Hern, Han Ho Jae

机构信息

Department of Veterinary Physiology, Biotherapy Human Resources Center (BK 21), College of Veterinary Medicine, Chonnam National University, Gwangju 500-757, Korea.

出版信息

J Cell Biochem. 2008 Aug 1;104(5):1598-611. doi: 10.1002/jcb.21657.

DOI:10.1002/jcb.21657

PMID:18646054

Abstract

Less information is available concerning the molecular mechanisms of cell survival after hypoxia in hepatocytes. Therefore, this study examined the effect of hypoxia on DNA synthesis and its related signal cascades in primary cultured chicken hepatocytes. Hypoxia increased [3H] thymidine incorporation, which was increased significantly after 0-24 h of hypoxic exposure. Indeed, the percentage of cell population in the S phase was increased in hypoxia condition. However, the release of LDH indicating cellular injury was not changed under hypoxic conditions. Hypoxia increased Ca2+ uptake and PKC translocation from the cytosol to the membrane fraction. Among the PKC isoforms, hypoxia stimulated the translocation of PKC alpha and epsilon. Hypoxia also phosphorylated the p38 and p44/42 mitogen-activated protein kinases (MAPKs), which were blocked by the inhibition of PKC. On the other hand, hypoxia increased Akt and mTOR phosphorylation, which was blocked in the absence of intra/extracellular Ca2+. The inhibition of PKC/MAPKs or PI3K/Akt pathway blocked the hypoxia-induced [3H] thymidine incorporation. However, hypoxia-induced Ca2+ uptake and PKC translocation was not influenced by LY 294002 or Akt inhibitor and hypoxia-induced MAPKs phosphorylation was not changed by rapamycin. In addition, LY 294002 or Akt inhibitor has no effect on the phosphorylation of MAPKs. It suggests that there is no direct interaction between the two pathways, which cooperatively mediated cell cycle progression to hypoxia in chicken hepatocytes. Hypoxia also increased the level of the cell cycle regulatory proteins [cyclin D(1), cyclin E, cyclin-dependent kinase (CDK) 2, and CDK 4] and p-RB protein but decreased the p21 and p27 expression levels, which were blocked by inhibitors of upstream signal molecules. In conclusion, short time exposure to hypoxia increases DNA synthesis in primary cultured chicken hepatocytes through cooperation of Ca2+/PKC, p38 MAPK, p44/42 MAPKs, and PI3K/Akt pathways.

摘要

关于肝细胞缺氧后细胞存活的分子机制，目前所知信息较少。因此，本研究检测了缺氧对原代培养鸡肝细胞DNA合成及其相关信号级联反应的影响。缺氧增加了[³H]胸苷掺入，在缺氧暴露0 - 24小时后显著增加。实际上，在缺氧条件下S期细胞群体的百分比增加。然而，表明细胞损伤的乳酸脱氢酶释放量在缺氧条件下没有变化。缺氧增加了Ca²⁺摄取以及蛋白激酶C（PKC）从胞质溶胶向膜部分的转位。在PKC亚型中，缺氧刺激了PKCα和ε的转位。缺氧还使p38和p44/42丝裂原活化蛋白激酶（MAPK）磷酸化，这被PKC的抑制所阻断。另一方面，缺氧增加了Akt和mTOR磷酸化，在缺乏细胞内/外Ca²⁺的情况下被阻断。PKC/MAPK或PI3K/Akt途径的抑制阻断了缺氧诱导的[³H]胸苷掺入。然而，缺氧诱导的Ca²⁺摄取和PKC转位不受LY 294002或Akt抑制剂的影响，缺氧诱导的MAPK磷酸化不受雷帕霉素的影响。此外，LY 294002或Akt抑制剂对MAPK的磷酸化没有影响。这表明这两条途径之间没有直接相互作用，它们协同介导鸡肝细胞对缺氧的细胞周期进程。缺氧还增加了细胞周期调节蛋白[细胞周期蛋白D（1）、细胞周期蛋白E、细胞周期蛋白依赖性激酶（CDK）2和CDK 4]以及p - RB蛋白的水平，但降低了p21和p27的表达水平，这被上游信号分子抑制剂所阻断。总之，短时间暴露于缺氧通过Ca²⁺/PKC、p38 MAPK、p44/42 MAPK和PI3K/Akt途径的协同作用增加原代培养鸡肝细胞中的DNA合成。

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原代培养鸡肝细胞短期缺氧诱导DNA合成的潜在机制：Ca(2+)/PKC/MAPKs与PI3K/Akt/mTOR之间的相关性

A potential mechanism for short time exposure to hypoxia-induced DNA synthesis in primary cultured chicken hepatocytes: Correlation between Ca(2+)/PKC/MAPKs and PI3K/Akt/mTOR.

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