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自噬相关基因 14(Atg14)受叉头框 O 转录因子和昼夜节律调节,在肝脏自噬和脂质代谢中发挥关键作用。

The autophagy-related gene 14 (Atg14) is regulated by forkhead box O transcription factors and circadian rhythms and plays a critical role in hepatic autophagy and lipid metabolism.

机构信息

Department of Biochemistry and Molecular Biology, Indiana University School of Medicine, Indianapolis, Indiana 46202, USA.

出版信息

J Biol Chem. 2012 Nov 9;287(46):39107-14. doi: 10.1074/jbc.M112.412569. Epub 2012 Sep 19.

Abstract

Autophagy plays a critical role in cell survival from prolonged starvation and recycling of aggregated proteins and damaged organelles. One of the essential genes involved in the autophagic initiation is autophagy-related 14 (Atg14), also called Barkor for Beclin 1-associated autophagy-related key regulator. Although its crucial role in the autophagic process has been reported, the gene regulation of Atg14 and its metabolic functions remain unclear. In this work we have identified that the Atg14 gene is regulated by forkhead box O (FoxO) transcription factors and circadian rhythms in the mouse liver. Luciferase reporter analyses and chromatin immunoprecipitation assays have revealed well conserved cis-elements for FoxOs and Clock/Bmal1 in the proximal promoter of the Atg14 gene. To examine the functions of hepatic Atg14, we have performed the gene knockdown and overexpression in the mouse livers. Remarkably, knockdown of Atg14 leads to elevated levels of triglycerides in the liver and serum as well. Conversely, overexpression of Atg14 improves hypertriglyceridemia in both high fat diet-treated wild-type mice and FoxO1/3/4 liver-specific knock-out mice. In summary, our data suggest that Atg14 is a new target gene of FoxOs and the core clock machinery, and this gene plays an important role in hepatic lipid metabolism.

摘要

自噬在细胞从长期饥饿中存活和回收聚集的蛋白质和受损的细胞器中起着关键作用。参与自噬起始的必需基因之一是自噬相关蛋白 14(Atg14),也称为 Beclin 1 相关自噬相关关键调节因子 Barkor。尽管已经报道了其在自噬过程中的重要作用,但 Atg14 的基因调控及其代谢功能仍不清楚。在这项工作中,我们已经确定 Atg14 基因受到叉头框 O(FoxO)转录因子和小鼠肝脏中昼夜节律的调节。荧光素酶报告分析和染色质免疫沉淀分析揭示了 Atg14 基因近端启动子中 FoxO 和 Clock/Bmal1 的保守顺式元件。为了研究肝组织 Atg14 的功能,我们在小鼠肝脏中进行了基因敲低和过表达实验。值得注意的是,Atg14 的敲低导致肝脏和血清中的甘油三酯水平升高。相反,Atg14 的过表达可改善高脂肪饮食处理的野生型小鼠和 FoxO1/3/4 肝特异性敲除小鼠的高甘油三酯血症。总之,我们的数据表明 Atg14 是 FoxO 和核心时钟机制的新靶基因,该基因在肝脏脂质代谢中起着重要作用。

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