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肝脏特异性组蛋白去乙酰化酶3缺失会破坏代谢转录网络。

Liver-specific deletion of histone deacetylase 3 disrupts metabolic transcriptional networks.

作者信息

Knutson Sarah K, Chyla Brenda J, Amann Joseph M, Bhaskara Srividya, Huppert Stacey S, Hiebert Scott W

机构信息

Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, TN 37232, USA.

出版信息

EMBO J. 2008 Apr 9;27(7):1017-28. doi: 10.1038/emboj.2008.51. Epub 2008 Mar 20.

DOI:10.1038/emboj.2008.51
PMID:18354499
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2323257/
Abstract

Histone deacetylase 3 (Hdac3) is an enzymatic component of transcriptional repression complexes recruited by the nuclear hormone receptors. Inactivation of Hdac3 in cancer cell lines triggered apoptosis, and removal of Hdac3 in the germ line of mice caused embryonic lethality. Therefore, we deleted Hdac3 in the postnatal mouse liver. These mice developed hepatomegaly, which was the result of hepatocyte hypertrophy, and these morphological changes coincided with significant imbalances between carbohydrate and lipid metabolism. Loss of Hdac3 triggered changes in gene expression consistent with inactivation of repression mediated by nuclear hormone receptors. Loss of Hdac3 also increased the levels of Ppar gamma2, and treatment of these mice with a Ppar gamma antagonist partially reversed the lipid accumulation in the liver. In addition, gene expression analysis identified mammalian target of rapamycin signalling as being activated after deletion of Hdac3, and inhibition by rapamycin affected the accumulation of neutral lipids in Hdac3-null livers. Thus, Hdac3 regulates metabolism through multiple signalling pathways in the liver, and deletion of Hdac3 disrupts normal metabolic homeostasis.

摘要

组蛋白去乙酰化酶3(Hdac3)是核激素受体招募的转录抑制复合物的一种酶成分。癌细胞系中Hdac3的失活引发细胞凋亡,而小鼠生殖系中Hdac3的缺失导致胚胎致死。因此,我们在出生后的小鼠肝脏中删除了Hdac3。这些小鼠出现了肝肿大,这是肝细胞肥大的结果,并且这些形态学变化与碳水化合物和脂质代谢之间的显著失衡同时出现。Hdac3的缺失引发了与核激素受体介导的抑制失活一致的基因表达变化。Hdac3的缺失还增加了Ppar gamma2的水平,用Ppar gamma拮抗剂治疗这些小鼠可部分逆转肝脏中的脂质积累。此外,基因表达分析确定雷帕霉素信号通路的哺乳动物靶点在Hdac3缺失后被激活,雷帕霉素的抑制作用影响了Hdac3缺失肝脏中中性脂质的积累。因此,Hdac3通过肝脏中的多种信号通路调节代谢,Hdac3的缺失破坏了正常的代谢稳态。

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