Department of Molecular and Cellular Biology, Baylor College of Medicine, Houston, TX.
Integrative Molecular and Biomedical Sciences Graduate Program, Baylor College of Medicine, Houston, TX.
Hepatology. 2020 May;71(5):1559-1574. doi: 10.1002/hep.30937. Epub 2020 Feb 23.
Obesity-induced chronic inflammation is a key component in the pathogenesis of nonalcoholic fatty liver disease (NAFLD) and insulin resistance. Increased secretion of proinflammatory cytokines by macrophages in metabolic tissues promotes disease progression. In the diet-induced obesity (DIO) mouse model, activation of liver resident macrophages, or Kupffer cells (KCs), drives inflammatory responses, which recruits circulating macrophages and promotes fatty liver development, and ultimately contributes to impaired hepatic insulin sensitivity. Hepatic macrophages express the highest level of vitamin D receptors (VDRs) among nonparenchymal cells, whereas VDR expression is very low in hepatocytes. VDR activation exerts anti-inflammatory effects in immune cells.
Here we found that VDR activation exhibits strong anti-inflammatory effects in mouse hepatic macrophages, including those isolated from DIO livers, and mice with genetic loss of Vdr developed spontaneous hepatic inflammation at 6 months of age. Under the chronic inflammation conditions of the DIO model, VDR activation by the vitamin D analog calcipotriol reduced liver inflammation and hepatic steatosis, significantly improving insulin sensitivity. The hyperinsulinemic euglycemic clamp revealed that VDR activation greatly increased the glucose infusion rate, while hepatic glucose production was remarkably decreased. Glucose uptake in muscle and adipose did not show similar effects, suggesting that improved hepatic insulin sensitivity is the primary contributor to the beneficial effects of VDR activation. Finally, specifically ablating liver macrophages by treatment with clodronate liposomes largely abolished the beneficial metabolic effects of calcipotriol, confirming that VDR activation in liver macrophages is required for the antidiabetic effect.
Activation of liver macrophage VDRs by vitamin D ligands ameliorates liver inflammation, steatosis and insulin resistance. Our results suggest therapeutic paradigms for treatment of NAFLD and type 2 diabetes mellitus.
肥胖引起的慢性炎症是导致非酒精性脂肪性肝病(NAFLD)和胰岛素抵抗的关键因素。代谢组织中巨噬细胞促炎细胞因子的过度分泌会促进疾病的进展。在饮食诱导的肥胖(DIO)小鼠模型中,肝脏驻留巨噬细胞或库普弗细胞(KCs)的激活会驱动炎症反应,招募循环巨噬细胞并促进脂肪肝的发展,最终导致肝胰岛素敏感性受损。肝巨噬细胞在非实质细胞中表达最高水平的维生素 D 受体(VDR),而肝细胞中 VDR 表达水平非常低。VDR 激活在免疫细胞中发挥抗炎作用。
在这里,我们发现 VDR 激活在小鼠肝巨噬细胞中表现出很强的抗炎作用,包括从 DIO 肝脏中分离出的巨噬细胞,并且 Vdr 基因缺失的小鼠在 6 个月大时就会自发发生肝炎症。在 DIO 模型的慢性炎症条件下,维生素 D 类似物卡泊三醇激活 VDR 可减少肝脏炎症和肝脂肪变性,显著改善胰岛素敏感性。高胰岛素正葡萄糖钳夹实验表明,VDR 激活大大增加了葡萄糖输注率,而肝葡萄糖生成显著降低。肌肉和脂肪中的葡萄糖摄取没有表现出类似的效果,这表明改善的肝胰岛素敏感性是 VDR 激活有益作用的主要贡献者。最后,用氯膦酸盐脂质体特异性地耗竭肝巨噬细胞,在很大程度上消除了卡泊三醇的有益代谢作用,证实了 VDR 在肝巨噬细胞中的激活是抗糖尿病作用所必需的。
维生素 D 配体激活肝巨噬细胞 VDR 可改善肝脏炎症、脂肪变性和胰岛素抵抗。我们的研究结果为治疗非酒精性脂肪性肝病和 2 型糖尿病提供了治疗策略。
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