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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Akt-mediated foxo1 inhibition is required for liver regeneration
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Akt-mediated foxo1 inhibition is required for liver regeneration

机译:肝再生需要Akt介导的FoxO1抑制

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Understanding the hepatic regenerative process has clinical interest as the effectiveness of many treatments for chronic liver diseases is conditioned by efficient liver regeneration. Experimental evidence points to the need for a temporal coordination between cytokines, growth factors, and metabolic signaling pathways to enable successful liver regeneration. One intracellular mediator that acts as a signal integration node for these processes is the serine-threonine kinase Akt/protein kinase B (Akt). To investigate the contribution of Akt during hepatic regeneration, we performed partial hepatectomy in mice lacking Akt1, Akt2, or both isoforms. We found that absence of Akt1 or Akt2 does not influence liver regeneration after partial hepatectomy. However, hepatic-specific Akt1 and Akt2 null mice show impaired liver regeneration and increased mortality. The major abnormal cellular events observed in total Akt-deficient livers were a marked reduction in cell proliferation, cell hypertrophy, glycogenesis, and lipid droplet formation. Most importantly, liver-specific deletion of FoxO1, a transcription factor regulated by Akt, rescued the hepatic regenerative capability in Akt1-deficient and Akt2-deficient mice and normalized the cellular events associated with liver regeneration. Conclusion: The Akt-FoxO1 signaling pathway plays an essential role during liver regeneration. (Hepatology 2016;63:1660-1674)
机译:了解肝再生过程具有临床兴趣,随着许多治疗慢性肝病治疗的有效性,通过有效的肝再生调节。实验证据指出了细胞因子,生长因子和代谢信号传导途径之间的时间协调,以实现成功的肝再生。用作这些方法的信号积分节点的一个细胞内介体是丝氨酸苏氨酸激酶Akt /蛋白激酶B(akt)。为了探讨肝脏再生期间AKT的贡献,我们在缺乏AKT1,AKT2或两种同种型的小鼠中进行部分肝切除术。我们发现不存在AKT1或AKT2在部分肝切除术后不会影响肝脏再生。然而,肝特异性AKT1和AKT2含氟小鼠显示出肝再生损害和增加的死亡率。在总Akt缺陷型肝脏中观察到的主要异常细胞事件是细胞增殖,细胞肥大,糖细胞和脂质液滴形成的显着降低。最重要的是,FOXO1的肝脏特异性缺失是AKT调节的转录因子,抢救了AKT1缺陷和Akt2缺陷小鼠中的肝再生能力,并标准化与肝再生相关的细胞事件。结论:AKT-FOXO1信号通路在肝脏再生期间发挥重要作用。 (2016年肝脏学; 63:1660-1674)

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