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Postprandial Hepatic Lipid Metabolism Requires Signaling through Akt2 Independent of the Transcription Factors FoxA2, FoxO1, and SREBP1c

机译：餐后肝脏脂质代谢需要信号通过akt2独立于转录因子Foxa2，FoxO1和sREBp1c

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摘要

Under conditions of obesity and insulin resistance, the serine/threonine protein kinase Akt/PKB is required for lipid accumulation in liver. Two forkhead transcription factors, FoxA2 and FoxO1, have been suggested to function downstream of and to be negatively regulated by Akt and are proposed as key determinants of hepatic triglyceride content. In this study, we utilize genetic loss of function experiments to show that constitutive activation of neither FoxA2 nor FoxO1 can account for the protection from steatosis afforded by deletion of Akt2 in liver. Rather, another downstream target positively regulated by Akt, the mTORC1 complex, is required in vivo for de novo lipogenesis and Srebp1c expression. Nonetheless, activation of mTORC1 and SREBP1c is not sufficient to drive postprandial lipogenesis in the absence of Akt2. These data show that insulin signaling through Akt2 promotes anabolic lipid metabolism independent of Foxa2 or FoxO1 and through pathways additional to the mTORC1-dependent activation of SREBP1c.

机译：在肥胖和胰岛素抵抗的情况下，肝脏脂质的积累需要丝氨酸/苏氨酸蛋白激酶Akt / PKB。有人提出两个叉头转录因子FoxA2和FoxO1在Akt的下游起作用并受到Akt的负调控，并被提议作为肝甘油三酯含量的关键决定因素。在这项研究中，我们利用功能丧失的遗传实验来证明FoxA2和FoxO1的组成性激活都不能解释肝脏中Akt2缺失对脂肪变性的保护作用。相反，体内从头产生脂肪和表达Srebp1c时需要Akt积极调控的另一个下游靶标mTORC1复合物。但是，在缺少Akt2的情况下，mTORC1和SREBP1c的激活不足以驱动餐后脂肪生成。这些数据表明，通过Akt2进行的胰岛素信号传导可促进合成代谢脂质代谢，而与Foxa2或FoxO1无关，并通过依赖于mTORC1的SREBP1c激活途径得以促进。

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Wan, Min; Leavens, Karla F.; Saleh, Danish; Easton, Rachael M.; Guertin, David A.; Peterson, Timothy R.; Kaestner, Klaus H.; Sabatini, David M.; Birnbaum, Morris J.; Sabatini, David M.; Peterson, Timothy R.;
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1. Postprandial hepatic lipid metabolism requires signaling through Akt2 independent of the transcription factors FoxA2, FoxO1, and SREBP1c. [J] . Wan M, Leavens KF, Saleh D, Cell metabolism . 2011,第4期

机译：餐后肝脂质代谢需要独立于转录因子FoxA2，FoxO1和SREBP1c的Akt2发出信号。
2. PIASy-Mediated Sumoylation of SREBP1c Regulates Hepatic Lipid Metabolism upon Fasting Signaling [J] . Gha Young Lee, Hagoon Jang, Jae Ho Lee, Molecular and Cellular Biology . 2014,第6期

机译：PIASy介导的SREBP1c的糖基化调节禁食信号后的肝脂质代谢。
3. A floor plate enhancer of the zebrafish netrin1 gene requires Cyclops (Nodal) signalling and the winged helix transcription factor FoxA2 [J] . Rastegar S., Albert S., Le Roux I., Developmental biology . 2002,第1期

机译：斑马鱼netrin1基因的地板增强子需要Cyclops（Nodal）信号传导和翅螺旋转录因子FoxA2
4. FoxO1 Inhibits Sterol Regulatory Element-binding Protein-1c (SREBP-1c) Gene Expression via Transcription Factors SREBP-1c and LXR in Goat Mammary Epithelial Cells [C] . Q.Y.He, J.Luo, J.Wu The 6th International Symposium on Dairy Cow Nutrition and Milk Quality（第六届“奶牛营养与牛奶质量”国际研讨会）论文集 . -1

机译：FOXO1通过转录因子Srebp-1C和LXR抑制甾醇调节元素结合蛋白-1C（Sreb-1c）基因表达，山羊乳腺上皮细胞
5. The role of Akt2 in hepatic lipid metabolism [D] . Leavens, Karla F. 2010

机译：Akt2在肝脂质代谢中的作用
6. Postprandial Hepatic Lipid Metabolism Requires Signaling though Akt2 Independent of the Transcription Factors FoxA2 FoxO1 and SREBP1c [O] . Min Wan, Karla F. Leavens, Danish Saleh, -1

机译：餐后肝脏脂质代谢需要信令虽然转录的akt2的独立因素FOXa2FoxO1的和sREBp1c
7. Postprandial Hepatic Lipid Metabolism Requires Signaling through Akt2 Independent of the Transcription Factors FoxA2, FoxO1, and SREBP1c [O] . Wan Min, Leavens Karla F., Saleh Danish, 2011

机译：餐后肝脂质代谢需要通过Akt2进行信号传递，而不受转录因子FoxA2，FoxO1和SREBP1c的影响

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