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首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Cannabinoid Receptor Type 1 (CB1R) Signaling Regulates Hepatic Gluconeogenesis via Induction of Endoplasmic Reticulum-bound Transcription Factor cAMP-responsive Element-binding Protein H (CREBH) in Primary Hepatocytes
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Cannabinoid Receptor Type 1 (CB1R) Signaling Regulates Hepatic Gluconeogenesis via Induction of Endoplasmic Reticulum-bound Transcription Factor cAMP-responsive Element-binding Protein H (CREBH) in Primary Hepatocytes

机译:大麻素1型(CB1R)信号传导通过诱导内质网结合转录因子cAMP响应元件结合蛋白H(CREBH)调节肝糖原异生。

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Activated cannabinoid 1 receptor (CB1R) signaling has been implicated in the development of phenotypes associated with fatty liver, insulin resistance, and impaired suppression of hepatic glucose output. Endoplasmic reticulum stress-associated liver-specific transcription factor CREBH is emerging as a critical player in various hepatic metabolic pathways and regulates hepatic gluconeogenesis in diet-induced obese settings. In this study, we elucidated the critical role of CREBH in mediating CB1R signaling to regulate glucose homeostasis in primary rat and human hepatocytes. mRNA and protein levels and glucose production were analyzed in primary rat and human hepatocytes. ChIP assays were performed together with various transcriptional analyses using standard techniques. CB1R activation by 2-arachidonoylglycerol (2-AG) specifically induced CREBH gene expression via phosphorylation of the JNK signaling pathway and c-Jun binding to the AP-1 binding site in the CREBH gene promoter. 2-AG treatment significantly induced hepatic gluconeogenic gene expression and glucose production in primary hepatocytes, and we demonstrated that the CREBH binding site mutant significantly attenuated 2-AG-mediated activation of the gluconeogenic gene promoter. Endogenous knockdown of CREBH led to ablation of 2-AG-induced gluconeogenic gene expression and glucose production, and the CB1R antagonist AM251 or insulin exhibited repression of CREBH gene induction and subsequently inhibited gluconeogenesis in both rat and human primary hepatocytes. These results demonstrate a novel mechanism of action of activated CB1R signaling to induce hepatic gluconeogenesis via direct activation of CREBH, thereby contributing to a better understanding of the endocannabinoid signaling mechanism involved in regulating the hepatic glucose metabolism.
机译:激活的大麻素1受体(CB1R)信号传导与脂肪肝,胰岛素抵抗和肝葡萄糖输出抑制受损相关的表型发展有关。内质网应激相关的肝特异性转录因子CREBH在各种肝代谢途径中起着至关重要的作用,并在饮食诱导的肥胖环境中调节肝糖异生。在这项研究中,我们阐明了CREBH在介导CB1R信号传导调节原代大鼠和人类肝细胞葡萄糖稳态中的关键作用。在原代大鼠和人类肝细胞中分析了mRNA和蛋白质水平以及葡萄糖生成。使用标准技术,将ChIP分析与各种转录分析一起进行。 2-花生四烯酰甘油(2-AG)对CB1R的激活通过JNK信号通路的磷酸化和c-Jun与CREBH基因启动子中AP-1结合位点的结合特异性诱导CREBH基因表达。 2-AG处理显着诱导原代肝细胞中肝糖原异基因表达和葡萄糖生成,并且我们证明了CREBH结合位点突变体显着减弱了2-AG介导的糖原异基因启动子的激活。 CREBH的内源性敲除导致2-AG诱导的糖异生基因表达和葡萄糖生成的消融,并且CB1R拮抗剂AM251或胰岛素表现出CREBH基因诱导的抑制作用,并随后抑制了大鼠和人类原代肝细胞的糖异生。这些结果证明了活化的CB1R信号转导通过直接激活CREBH诱导肝糖异生的作用的新机制,从而有助于更好地了解参与调节肝糖代谢的内源性大麻素信号转导机制。

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