肝脂肪酶影响小鼠体内高密度脂蛋白和载脂蛋白水平

Sylvie Braschi , Nicole Couture , Adriana Gambarotta , Benoit R Gauthier , Cynthia R Coffill , Daniel L Sparks , Nobuyo Maeda , Joshua R Schultz
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引用次数: 34

摘要

利用转基因小鼠过量产生一系列人脂肪酶(hHL)活性(增加4 - 23倍),进一步研究肝脂肪酶(HL)在脂蛋白代谢中的作用。肝素释放型HL活性增加了5倍,并伴有中度(约1。血浆总胆固醇、高密度脂蛋白(HDL)胆固醇和磷脂(PL)降低20%,但甘油三酯(TG)无显著变化。HL活性增加23倍导致血浆总胆固醇和高密度脂蛋白胆固醇、PL和TG显著下降(分别为77%、64%、60%和24%),IDL、LDL和HDL组脂蛋白脂显著下降。高水平的HL活性降低了apoA-I、A-II和apoE的血浆浓度(分别为76%、48%和75%)。相反,含apoa - iv的脂蛋白水平似乎相对抵抗hHL活性滴度的增加。hHL活性的增加与LpAI和LpB48颗粒水平的逐渐下降和密度的增加有关。hHL转基因小鼠血浆中125i标记的人HDL消失率增加,表明转基因小鼠对HDL载脂蛋白的清除率增加。HL活性增加对载脂蛋白100的影响更为复杂。与对照组相比,hl缺陷小鼠含有载脂蛋白100的低密度脂蛋白(LDL)显著减少。HL活性的增加与脂蛋白密度谱的转变有关,从主要的浮力(VLDL/IDL)脂蛋白到更密集(LDL)的部分。HL活性从中等(4倍)增加到较高(5倍)水平,降低了含apob100颗粒的水平。因此,在小鼠正常至中等高水平时,HL促进了HDL和载脂蛋白的代谢,从而成为血浆中HDL和LDL水平的关键决定因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hepatic lipase affects both HDL and ApoB-containing lipoprotein levels in the mouse

Transgenic mice were created overproducing a range of human HL (hHL) activities (4–23-fold increase) to further examine the role of hepatic lipase (HL) in lipoprotein metabolism. A 5-fold increase in heparin releasable HL activity was accompanied by moderate (approx. 20%) decreases in plasma total and high density lipoprotein (HDL) cholesterol and phospholipid (PL) but no significant change in triglyceride (TG). A 23-fold increase in HL activity caused a more significant decrease in plasma total and HDL cholesterol, PL and TG (77%, 64%, 60%, and 24% respectively), and a substantial decrease in lipoprotein lipids amongst IDL, LDL and HDL fractions. High levels of HL activity diminished the plasma concentration of apoA-I, A-II and apoE (76%, 48% and 75%, respectively). In contrast, the levels of apoA-IV-containing lipoproteins appear relatively resistant to increased titers of hHL activity. Increased hHL activity was associated with a progressive decrease in the levels and an increase in the density of LpAI and LpB48 particles. The increased rate of disappearance of 125I-labeled human HDL from the plasma of hHL transgenic mice suggests increased clearance of HDL apoproteins in the transgenic mice. The effect of increased HL activity on apoB100-containing lipoproteins was more complex. HL-deficient mice have substantially decreased apoB100-containing low density lipoproteins (LDL) compared to controls. Increased HL activity is associated with a transformation of the lipoprotein density profile from predominantly buoyant (VLDL/IDL) lipoproteins to more dense (LDL) fractions. Increased HL activity from moderate (4-fold) to higher (5-fold) levels decreased the levels of apoB100-containing particles. Thus, at normal to moderately high levels in the mouse, HL promotes the metabolism of both HDL and apoB-containing lipoproteins and thereby acts as a key determinant of plasma levels of both HDL and LDL.

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