Activation of ER stress and mTORC1 suppresses hepatic sortilin-1 levels in obese mice
Ding Ai, … , Daniel J. Rader, Alan R. Tall
Ding Ai, … , Daniel J. Rader, Alan R. Tall
Published April 2, 2012
Citation Information: J Clin Invest. 2012;122(5):1677-1687. https://doi.org/10.1172/JCI61248.
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Activation of ER stress and mTORC1 suppresses hepatic sortilin-1 levels in obese mice

Abstract

Recent GWAS have identified SNPs at a human chromosom1 locus associated with coronary artery disease risk and LDL cholesterol levels. The SNPs are also associated with altered expression of hepatic sortilin-1 (SORT1), which encodes a protein thought to be involved in apoB trafficking and degradation. Here, we investigated the regulation of Sort1 expression in mouse models of obesity. Sort1 expression was markedly repressed in both genetic (ob/ob) and high-fat diet models of obesity; restoration of hepatic sortilin-1 levels resulted in reduced triglyceride and apoB secretion. Mouse models of obesity also exhibit increased hepatic activity of mammalian target of rapamycin complex 1 (mTORC1) and ER stress, and we found that administration of the mTOR inhibitor rapamycin to ob/ob mice reduced ER stress and increased hepatic sortilin-1 levels. Conversely, genetically increased hepatic mTORC1 activity was associated with repressed Sort1 and increased apoB secretion. Treating WT mice with the ER stressor tunicamycin led to marked repression of hepatic sortilin-1 expression, while administration of the chemical chaperone PBA to ob/ob mice led to amelioration of ER stress, increased sortilin-1 expression, and reduced apoB and triglyceride secretion. Moreover, the ER stress target Atf3 acted at the SORT1 promoter region as a transcriptional repressor, whereas knockdown of Atf3 mRNA in ob/ob mice led to increased hepatic sortilin-1 levels and decreased apoB and triglyceride secretion. Thus, in mouse models of obesity, induction of mTORC1 and ER stress led to repression of hepatic Sort1 and increased VLDL secretion via Atf3. This pathway may contribute to dyslipidemia in metabolic disease.

Authors

Ding Ai, Juan M. Baez, Hongfeng Jiang, Donna M. Conlon, Antonio Hernandez-Ono, Maria Frank-Kamenetsky, Stuart Milstein, Kevin Fitzgerald, Andrew J. Murphy, Connie W. Woo, Alanna Strong, Henry N. Ginsberg, Ira Tabas, Daniel J. Rader, Alan R. Tall

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Figure 6

Regulation of sortilin-1 by ER stress.

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Regulation of sortilin-1 by ER stress. (A) Western blot analysis of sort...
(A) Western blot analysis of sortilin-1 and Atf3 in cells of the McArdleH7777 line treated with DMSO or 5 μg/ml tunicamycin at the indicated time points. (B) Sort1 mRNA was determined by QPCR. McArdle cells were treated with DMSO control or 5 μg/ml tunicamycin or were preincubated with 5 μg/ml actinomycin D (ActD) for 30 minutes with or without 5 μg/ml tunicamycin for the indicated times. (C) Western blot analysis of sortilin-1 and Atf3 protein levels in McArdle cells treated with 1 μM thapsigargin (Tg) for the indicated times. (D) Grp78, Atf3, and Sort1 mRNA was measured by QPCR in McArdle cells treated with 1 μM thapsigargin for the indicated times. 3 separated experiments were performed. *P < 0.05 vs. control for the respective time point, unpaired t test.