肝核受体辅助抑制因子 1 通过 TRβ1 调控的途径调节胆固醇吸收。
Hepatic nuclear corepressor 1 regulates cholesterol absorption through a TRβ1-governed pathway.
出版信息
J Clin Invest. 2014 May;124(5):1976-86. doi: 10.1172/JCI73419. Epub 2014 Apr 8.
Abstract
Transcriptional coregulators are important components of nuclear receptor (NR) signaling machinery and provide additional mechanisms for modulation of NR activity. Expression of a mutated nuclear corepressor 1 (NCoR1) that lacks 2 NR interacting domains (NCoRΔID) in the liver leads to elevated expression of genes regulated by thyroid hormone receptor (TR) and liver X receptor (LXR), both of which control hepatic cholesterol metabolism. Here, we demonstrate that expression of NCoRΔID in mouse liver improves dietary cholesterol tolerance in an LXRα-independent manner. NCoRΔID-associated cholesterol tolerance was primarily due to diminished intestinal cholesterol absorption as the result of changes in the composition and hydrophobicity of the bile salt pool. Alterations of the bile salt pool were mediated by increased expression of genes encoding the bile acid metabolism enzymes CYP27A1 and CYP3A11 as well as canalicular bile salt pump ABCB11. We have determined that these genes are regulated by thyroid hormone and that TRβ1 is recruited to their regulatory regions. Together, these data indicate that interactions between NCoR1 and TR control a specific pathway involved in regulation of cholesterol metabolism and clearance.
摘要
转录共激活因子是核受体 (NR) 信号机制的重要组成部分,为 NR 活性的调节提供了额外的机制。在肝脏中表达缺失 2 个 NR 相互作用结构域 (NCoRΔID) 的突变核共抑制因子 1 (NCoR1),会导致受甲状腺激素受体 (TR) 和肝 X 受体 (LXR) 调控的基因表达升高,这两者都控制着肝脏胆固醇代谢。在这里,我们证明了 NCoRΔID 在小鼠肝脏中的表达以不依赖于 LXRα 的方式改善了饮食胆固醇耐受性。NCoRΔID 相关的胆固醇耐受性主要归因于肠道胆固醇吸收的减少,这是由于胆汁盐池的组成和疏水性发生了变化。胆汁盐池的改变是通过增加编码胆汁酸代谢酶 CYP27A1 和 CYP3A11 以及胆小管胆汁盐泵 ABCB11 的基因的表达来介导的。我们已经确定这些基因受甲状腺激素的调节,并且 TRβ1 被招募到它们的调节区域。综上所述,这些数据表明 NCoR1 和 TR 之间的相互作用控制了参与胆固醇代谢和清除的特定途径。
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