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本文引用的文献

1
The nuclear receptor constitutive active/androstane receptor arrests DNA-damaged human hepatocellular carcinoma Huh7 cells at the G2/M phase.核受体组成型激活/雄激素受体将受损的人肝癌 Huh7 细胞阻滞在 G2/M 期。
Mol Carcinog. 2012 Feb;51(2):206-12. doi: 10.1002/mc.20783. Epub 2011 May 6.
2
Nuclear receptor CAR represses TNFalpha-induced cell death by interacting with the anti-apoptotic GADD45B.核受体 CAR 通过与抗细胞凋亡蛋白 GADD45B 相互作用来抑制 TNFalpha 诱导的细胞死亡。
PLoS One. 2010 Apr 12;5(4):e10121. doi: 10.1371/journal.pone.0010121.
3
Dephosphorylation of threonine 38 is required for nuclear translocation and activation of human xenobiotic receptor CAR (NR1I3).苏氨酸 38 的去磷酸化对于人源异生物质受体 CAR(NR1I3)的核转位和激活是必需的。
J Biol Chem. 2009 Dec 11;284(50):34785-92. doi: 10.1074/jbc.M109.048108. Epub 2009 Oct 26.
4
Activation of nuclear receptor CAR ameliorates diabetes and fatty liver disease.核受体CAR的激活可改善糖尿病和脂肪肝疾病。
Proc Natl Acad Sci U S A. 2009 Nov 3;106(44):18831-6. doi: 10.1073/pnas.0909731106. Epub 2009 Oct 22.
5
PXR and CAR in energy metabolism.孕烷X受体和组成型雄烷受体与能量代谢
Trends Endocrinol Metab. 2009 Aug;20(6):273-9. doi: 10.1016/j.tem.2009.03.003.
6
Expression of CAR in SW480 and HepG2 cells during G1 is associated with cell proliferation.G1期SW480和HepG2细胞中CAR的表达与细胞增殖相关。
Biochem Biophys Res Commun. 2008 May 16;369(4):1027-33. doi: 10.1016/j.bbrc.2008.02.140. Epub 2008 Mar 10.
7
The roles of nuclear receptors CAR and PXR in hepatic energy metabolism.核受体CAR和PXR在肝脏能量代谢中的作用。
Drug Metab Pharmacokinet. 2008;23(1):8-13. doi: 10.2133/dmpk.23.8.
8
Extracellular signal-regulated kinase is an endogenous signal retaining the nuclear constitutive active/androstane receptor (CAR) in the cytoplasm of mouse primary hepatocytes.细胞外信号调节激酶是一种内源性信号,可将核组成型活性/雄烷受体(CAR)保留在小鼠原代肝细胞的细胞质中。
Mol Pharmacol. 2007 May;71(5):1217-21. doi: 10.1124/mol.107.034538. Epub 2007 Feb 21.
9
A physiological role of AMP-activated protein kinase in phenobarbital-mediated constitutive androstane receptor activation and CYP2B induction.AMP 活化蛋白激酶在苯巴比妥介导的组成型雄甾烷受体激活及 CYP2B 诱导中的生理作用。
Biochem J. 2007 Feb 1;401(3):735-41. doi: 10.1042/BJ20061238.
10
Stimulation of AMP-activated protein kinase is essential for the induction of drug metabolizing enzymes by phenobarbital in human and mouse liver.在人和小鼠肝脏中,激活AMP活化蛋白激酶对于苯巴比妥诱导药物代谢酶至关重要。
Mol Pharmacol. 2006 Dec;70(6):1925-34. doi: 10.1124/mol.106.029421. Epub 2006 Sep 20.

活性 ERK1/2 蛋白与磷酸化的核组成型激活/雄激素受体(CAR;NR1I3)相互作用,抑制磷酸化和将 CAR 隔离在细胞质中。

Active ERK1/2 protein interacts with the phosphorylated nuclear constitutive active/androstane receptor (CAR; NR1I3), repressing dephosphorylation and sequestering CAR in the cytoplasm.

机构信息

Pharmacogenetics Section, Laboratory of Reproductive and Developmental Toxicology, NIEHS, National Institutes of Health, Research Triangle Park, North Carolina 27709.

Pharmacogenetics Section, Laboratory of Reproductive and Developmental Toxicology, NIEHS, National Institutes of Health, Research Triangle Park, North Carolina 27709.

出版信息

J Biol Chem. 2011 Oct 14;286(41):35763-35769. doi: 10.1074/jbc.M111.284596. Epub 2011 Aug 26.

DOI:10.1074/jbc.M111.284596
PMID:21873423
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3195598/
Abstract

The nuclear constitutive active/androstane receptor (CAR) is inactivated and sequestered in the cytoplasm when Thr-38 is phosphorylated. Here, we have demonstrated that activated ERK1/2 interacts with phosphorylated CAR to repress dephosphorylation of Thr-38. The phosphorylation-dependent interaction between CAR and ERK1/2 was examined by co-immunoprecipitation experiments of ectopically expressed FLAG-tagged CAR T38A and CAR T38D mutants with endogenous phospho-ERK1/2 in Huh-7 cells. Phospho-ERK1/2 coprecipitated only the phosphorylation-mimicking CAR T38D mutant; this coprecipitation was mediated by the interaction with the xenochemical response signal peptide near the C terminus of CAR. This interaction increased after EGF treatment and decreased after treatment with the MEK inhibitor U0126 as well as after knockdown of MEK1/2 by shRNA in Huh-7 cells. The phosphorylation levels of Thr-38 of CAR decreased in U0126-treated Huh-7 cells. Thus, activated ERK1/2 interacts with CAR and represses dephosphorylation of Thr-38, providing a cell signal-regulated mechanism for CAR activation.

摘要

当 Thr-38 磷酸化时,核组成型激活的/雄激素受体 (CAR) 会失活并被隔离在细胞质中。在这里,我们已经证明,激活的 ERK1/2 与磷酸化的 CAR 相互作用,以抑制 Thr-38 的去磷酸化。通过在 Huh-7 细胞中外源表达的 FLAG 标记的 CAR T38A 和 CAR T38D 突变体与内源性磷酸化 ERK1/2 的共免疫沉淀实验,检查了 CAR 和 ERK1/2 之间磷酸化依赖性的相互作用。只有磷酸化模拟的 CAR T38D 突变体能与磷酸化的 ERK1/2 共沉淀;这种共沉淀是通过 CAR 近 C 末端的异种化学反应信号肽与 ERK1/2 的相互作用介导的。这种相互作用在 EGF 处理后增加,在用 MEK 抑制剂 U0126 处理以及在 Huh-7 细胞中用 shRNA 敲低 MEK1/2 后减少。在 U0126 处理的 Huh-7 细胞中,CAR 的 Thr-38 磷酸化水平降低。因此,激活的 ERK1/2 与 CAR 相互作用并抑制 Thr-38 的去磷酸化,为 CAR 的激活提供了一种细胞信号调节机制。