Department of Pathology, Northwestern University Feinberg School of Medicine, Chicago, IL, 60611, USA.
State Key Laboratory of Proteomics, Beijing Proteome Research Center, National Center for Protein Sciences (Beijing), Beijing Institute of Lifeomics, 102206, Beijing, China.
Nat Commun. 2018 Sep 10;9(1):3659. doi: 10.1038/s41467-018-06091-7.
The HMG-CoA reductase degradation protein 1 (HRD1) has been identified as a key enzyme for endoplasmic reticulum-associated degradation of misfolded proteins, but its organ-specific physiological functions remain largely undefined. Here we show that mice with HRD1 deletion specifically in the liver display increased energy expenditure and are resistant to HFD-induced obesity and liver steatosis and insulin resistance. Proteomic analysis identifies a HRD1 interactome, a large portion of which includes metabolic regulators. Loss of HRD1 results in elevated ENTPD5, CPT2, RMND1, and HSD17B4 protein levels and a consequent hyperactivation of both AMPK and AKT pathways. Genome-wide mRNA sequencing revealed that HRD1-deficiency reprograms liver metabolic gene expression profiles, including suppressing genes involved in glycogenesis and lipogenesis and upregulating genes involved in glycolysis and fatty acid oxidation. We propose HRD1 as a liver metabolic regulator and a potential drug target for obesity, fatty liver disease, and insulin resistance associated with the metabolic syndrome.
HMG-CoA 还原酶降解蛋白 1(HRD1)已被鉴定为内质网相关降解错误折叠蛋白的关键酶,但它在特定器官中的生理功能仍很大程度上未被定义。在这里,我们显示 HRD1 在肝脏中特异性缺失的小鼠表现出增加的能量消耗,并且对 HFD 诱导的肥胖、肝脂肪变性和胰岛素抵抗具有抗性。蛋白质组学分析确定了 HRD1 的相互作用组,其中很大一部分包括代谢调节剂。HRD1 的缺失导致 ENTAPD5、CPT2、RMND1 和 HSD17B4 蛋白水平升高,并且 AMPK 和 AKT 途径的过度激活。全基因组 mRNA 测序显示,HRD1 缺陷重新编程肝脏代谢基因表达谱,包括抑制参与糖生成和脂生成的基因,并上调参与糖酵解和脂肪酸氧化的基因。我们提出 HRD1 作为肝脏代谢调节剂和代谢综合征相关肥胖、脂肪肝疾病和胰岛素抵抗的潜在药物靶点。
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