Division of Gastroenterology, University of Pennsylvania, Philadelphia, PA.
Division of Gastroenterology, United Health Services, Binghamton, NY.
J Lipid Res. 2020 Jul;61(7):983-994. doi: 10.1194/jlr.RA119000446. Epub 2020 May 12.
Alcohol's impairment of both hepatic lipid metabolism and insulin resistance (IR) are key drivers of alcoholic steatosis, the initial stage of alcoholic liver disease (ALD). Pharmacologic reduction of lipotoxic ceramide prevents alcoholic steatosis and glucose intolerance in mice, but potential off-target effects limit its strategic utility. Here, we employed a hepatic-specific acid ceramidase (ASAH) overexpression model to reduce hepatic ceramides in a Lieber-DeCarli model of experimental alcoholic steatosis. We examined effects of alcohol on hepatic lipid metabolism, body composition, energy homeostasis, and insulin sensitivity as measured by hyperinsulinemic-euglycemic clamp. Our results demonstrate that hepatic ceramide reduction ameliorates the effects of alcohol on hepatic lipid droplet (LD) accumulation by promoting VLDL secretion and lipophagy, the latter of which involves ceramide cross-talk between the lysosomal and LD compartments. We additionally demonstrate that hepatic ceramide reduction prevents alcohol's inhibition of hepatic insulin signaling. These effects on the liver are associated with a reduction in oxidative stress markers and are relevant to humans, as we observe peri- LD ASAH expression in human ALD. Together, our results suggest a potential role for hepatic ceramide inhibition in preventing ALD.
酒精对肝脂质代谢和胰岛素抵抗(IR)的损害是酒精性脂肪变性的关键驱动因素,酒精性脂肪变性是酒精性肝病(ALD)的初始阶段。药理降低脂毒性神经酰胺可预防小鼠的酒精性脂肪变性和葡萄糖不耐受,但潜在的脱靶效应限制了其战略效用。在这里,我们使用肝特异性酸性神经酰胺酶(ASAH)过表达模型,在实验性酒精性脂肪变性的 Lieber-DeCarli 模型中降低肝神经酰胺。我们研究了酒精对肝脂质代谢、身体成分、能量平衡和胰岛素敏感性的影响,这些影响通过高胰岛素-正常血糖钳夹来衡量。我们的结果表明,肝神经酰胺的减少通过促进 VLDL 分泌和脂自噬来改善酒精对肝脂肪滴(LD)积累的影响,后者涉及溶酶体和 LD 隔室之间的神经酰胺串扰。我们还证明,肝神经酰胺的减少可防止酒精抑制肝胰岛素信号。这些对肝脏的影响与氧化应激标志物的减少有关,与人类有关,因为我们在人类 ALD 中观察到 LD 周围的 ASAH 表达。总之,我们的结果表明,肝神经酰胺抑制在预防 ALD 方面可能具有潜在作用。
