Swiatek Wojciech, Parnell K Mark, Nickols G Allen, Scharschmidt Bruce F, Rutter Jared
Department of Biochemistry University of Utah School of Medicine University of Utah Salt Lake City UT.
BioEnergenix, LLC San Francisco CA.
Hepatol Commun. 2020 Mar 24;4(5):696-707. doi: 10.1002/hep4.1498. eCollection 2020 May.
Hyperactivation of sterol regulatory element binding protein 1c (SREBP-1c), which transcriptionally induces expression of enzymes responsible for lipogenesis and triglyceride (TG) formation, is implicated in nonalcoholic fatty liver disease (NAFLD)/nonalcoholic steatohepatitis (NASH) pathogenesis. Posttranslational SREBP-1c maturation and activation is stimulated by the protein per-arnt-sim kinase (PASK). knockout mice are phenotypically normal on a conventional diet but exhibit decreased hypertriglyceridemia, insulin resistance, and hepatic steatosis on a high-fat diet. We investigated the effects of pharmacologic PASK inhibition using BioE-1115, a selective and potent oral PASK inhibitor, in Zucker fatty () rats, a genetic model of obesity, dyslipidemia, and insulin resistance, and in a dietary murine model of NAFLD/NASH. Female Zucker () rats and lean littermate (/+) controls received BioE-1115 (3-100 mg/kg/day) and/or omega-3 fatty acids, and blood glucose, hemoglobin A1c, glucose tolerance, insulin, and serum TG were measured. C57BL/6J mice fed a high-fat/high-fructose diet (HF-HFrD) were treated with BioE-1115 (100 mg/kg/day) or vehicle. Body weight and fasting glucose were measured regularly; serum TG, body and organ weights, and liver TG and histology were assessed at sacrifice. Messenger RNA (mRNA) abundance of SREBP-1c target genes was measured in both models. In Zucker rats, BioE-1115 treatment produced significant dose-dependent reductions in blood glucose, insulin, and TG (all greater than omega-3 fatty acids) and dose dependently restored insulin sensitivity assessed by glucose tolerance testing. In HF-HFrD mice, BioE-1115 reduced body weight, liver weight, fasting blood glucose, serum TGs, hepatic TG, hepatic fibrosis, hepatocyte vacuolization, and bile duct hyperplasia. BioE-1115 reduced SREBP-1c target mRNA transcripts in both models. PASK inhibition mitigates many adverse metabolic consequences associated with an HF-HFrD and reduces hepatic fat content and fibrosis. This suggests that inhibition of PASK is an attractive therapeutic strategy for NAFLD/NASH treatment.
甾醇调节元件结合蛋白1c(SREBP-1c)的过度激活在非酒精性脂肪性肝病(NAFLD)/非酒精性脂肪性肝炎(NASH)的发病机制中起作用,它可转录诱导负责脂肪生成和甘油三酯(TG)形成的酶的表达。蛋白芳香烃受体核转运蛋白样激酶(PASK)可刺激SREBP-1c的翻译后成熟和激活。PASK基因敲除小鼠在常规饮食条件下表现正常,但在高脂饮食时,其高甘油三酯血症、胰岛素抵抗和肝脂肪变性有所减轻。我们使用选择性强效口服PASK抑制剂BioE-1115,在肥胖、血脂异常和胰岛素抵抗的遗传模型Zucker脂肪(fa/fa)大鼠以及NAFLD/NASH饮食小鼠模型中研究了PASK药理抑制的作用。雌性Zucker(fa/fa)大鼠和瘦同窝对照(+/+)接受BioE-1115(3 - 100mg/kg/天)和/或ω-3脂肪酸,并测量血糖、糖化血红蛋白A1c、葡萄糖耐量、胰岛素和血清TG。给喂食高脂/高果糖饮食(HF-HFrD)的C57BL/6J小鼠用BioE-1115(100mg/kg/天)或赋形剂处理。定期测量体重和空腹血糖;处死时评估血清TG、体重和器官重量以及肝脏TG和组织学。在两个模型中均测量了SREBP-1c靶基因的信使核糖核酸(mRNA)丰度。在Zucker大鼠中,BioE-1115处理使血糖、胰岛素和TG显著剂量依赖性降低(均大于ω-3脂肪酸),并通过葡萄糖耐量试验剂量依赖性恢复胰岛素敏感性。在HF-HFrD小鼠中,BioE-1115降低了体重、肝脏重量、空腹血糖、血清TG、肝脏TG、肝纤维化、肝细胞空泡化和胆管增生。BioE-1115在两个模型中均降低了SREBP-1c靶mRNA转录本。PASK抑制减轻了与HF-HFrD相关的许多不良代谢后果,并降低了肝脏脂肪含量和纤维化。这表明抑制PASK是一种有吸引力的NAFLD/NASH治疗策略。
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