Diabetic and dyslipidaemic morbidly obese exhibit more liver alterations compared with healthy morbidly obese

Eva Pardina , Roser Ferrer , Joana Rossell , Juan Antonio Baena-Fustegueras , Albert Lecube , Jose Manuel Fort , Enric Caubet , Óscar González , Ramón Vilallonga , Víctor Vargas , José María Balibrea , Julia Peinado-Onsurbe
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引用次数: 11

Abstract

Background & aims

To study the origin of fat excess in the livers of morbidly obese (MO) individuals, we analysed lipids and lipases in both plasma and liver and genes involved in lipid transport, or related with, in that organ.

Methods

Thirty-two MO patients were grouped according to the absence (healthy: DM  DL −) or presence of comorbidities (dyslipidemic: DM  DL +; or dyslipidemic with type 2 diabetes: DM + DL +) before and one year after gastric bypass.

Results

The livers of healthy, DL and DM patients contained more lipids (9.8, 9.5 and 13.7 times, respectively) than those of control subjects. The genes implicated in liver lipid uptake, including HL, LPL, VLDLr, and FAT/CD36, showed increased expression compared with the controls. The expression of genes involved in lipid-related processes outside of the liver, such as apoB, PPARα and PGC1α, CYP7a1 and HMGCR, was reduced in these patients compared with the controls. PAI1 and TNFα gene expression in the diabetic livers was increased compared with the other obese groups and control group. Increased steatosis and fibrosis were also noted in the MO individuals.

Conclusions

Hepatic lipid parameters in MO patients change based on their comorbidities. The gene expression and lipid levels after bariatric surgery were less prominent in the diabetic patients. Lipid receptor overexpression could enable the liver to capture circulating lipids, thus favouring the steatosis typically observed in diabetic and dyslipidaemic MO individuals.

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与健康的病态肥胖相比,糖尿病和血脂异常的病态肥胖表现出更多的肝脏改变
背景,为了研究病态肥胖(MO)个体肝脏脂肪过量的起源,我们分析了血浆和肝脏中的脂质和脂肪酶以及参与脂质转运或与该器官相关的基因。方法32例MO患者根据有无(健康:DM−DL−)或是否存在合并症(血脂异常:DM−DL +;或血脂异常合并2型糖尿病(DM + DL +)。结果健康组、DL组和DM组肝脏脂质含量分别为对照组的9.8倍、9.5倍和13.7倍。与对照组相比,与肝脏脂质摄取相关的基因,包括HL、LPL、VLDLr和FAT/CD36的表达增加。与对照组相比,这些患者肝外参与脂质相关过程的基因,如apoB、PPARα和PGC1α、CYP7a1和HMGCR的表达降低。与其他肥胖组和对照组相比,糖尿病患者肝脏中PAI1和TNFα基因表达升高。在MO个体中也注意到脂肪变性和纤维化的增加。结论MO患者的肝脂质参数随其合并症而变化。糖尿病患者减肥手术后的基因表达和血脂水平不明显。脂质受体过表达可以使肝脏捕获循环脂质,从而有利于在糖尿病和血脂异常的MO个体中典型观察到的脂肪变性。
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