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人卵磷脂胆固醇酰基转移酶在转基因小鼠中的表达。人载脂蛋白AI和人载脂蛋白AII对血浆脂蛋白胆固醇代谢的影响。

Expression of human lecithin-cholesterol acyltransferase in transgenic mice. Effect of human apolipoprotein AI and human apolipoprotein all on plasma lipoprotein cholesterol metabolism.

作者信息

Francone O L, Gong E L, Ng D S, Fielding C J, Rubin E M

机构信息

Cardiovascular Research Institute, University of California Medical Center, San Francisco 94143, USA.

出版信息

J Clin Invest. 1995 Sep;96(3):1440-8. doi: 10.1172/JCI118180.

Abstract

Human (Hu) lecithin-cholesterol acyltransferase (LCAT) is a key enzyme in the plasma metabolism of cholesterol. To assess the effects of increased plasma levels of LCAT, four lines of transgenic mice were created expressing a Hu LCAT gene driven by either its natural or the mouse albumin enhancer promoter. Plasma LCAT activity increased from 1.2- to 1.6-fold higher than that found in control mouse plasma. Lipid profiles, upon comparing Hu LCAT transgenics to control animals, revealed a 20 t0 60% increase in total and cholesteryl esters that were mainly present in HDL. The in vivo substrate specificity of Hu LCAT was assessed by creating animals expressing Hu apo AI + Hu LCAT (HuAI/ LCAT), Hu apo AI + Hu apo AII + Hu LCAT (HuAI/ AII/LCAT), and Hu apo AII + Hu LCAT (HuAII/LCAT). Plasma cholesterol was increased up to 4.2-fold in HuAI/ LCAT transgenic mice and twofold in the HuAI/AII/LCAT transgenic mice, compared with HuAI and HuAI/AII transgenic mice. HDL cholesteryl ester levels were increased more than twofold in both the HuAI/LCAT and HuAI/AII/LCAT mice compared with the HuAI, HuAI/AII, and HuLCAT animals. The HDL particles were predominantly larger in the HuAI/LCAT and the HuAI/AII/LCAT mice compared with those in HuAI, HuAII/LCAT, and HuLCAT animals. The increase in LCAT activity in the HuAI/LCAT and HuAI/AII/LCAT mice was associated with 62 and 27% reductions respectively, in the proportion of Hu apo AI in the pre beta-HDL fraction, when compared with HuAI and HuAI/AII transgenic mice. These data demonstrate that moderate increases in LCAT activity are associated with significant changes in lipoprotein cholesterol levels and that Hu LCAT has a significant preference for HDL containing Hu apo AI.

摘要

人源(Hu)卵磷脂胆固醇酰基转移酶(LCAT)是血浆胆固醇代谢中的关键酶。为了评估血浆中LCAT水平升高的影响,构建了四条转基因小鼠品系,它们分别由天然启动子或小鼠白蛋白增强子启动子驱动表达Hu LCAT基因。与对照小鼠血浆相比,转基因小鼠血浆LCAT活性提高了1.2至1.6倍。将Hu LCAT转基因小鼠与对照动物的血脂谱进行比较,发现主要存在于高密度脂蛋白(HDL)中的总胆固醇酯和胆固醇酯增加了20%至60%。通过构建表达Hu载脂蛋白AI + Hu LCAT(HuAI/LCAT)、Hu载脂蛋白AI + Hu载脂蛋白AII + Hu LCAT(HuAI/AII/LCAT)和Hu载脂蛋白AII + Hu LCAT(HuAII/LCAT)的动物来评估Hu LCAT在体内的底物特异性。与HuAI和HuAI/AII转基因小鼠相比,HuAI/LCAT转基因小鼠的血浆胆固醇增加了4.2倍,HuAI/AII/LCAT转基因小鼠增加了两倍。与HuAI、HuAI/AII和HuLCAT动物相比,HuAI/LCAT和HuAI/AII/LCAT小鼠的HDL胆固醇酯水平均增加了两倍多。与HuAI、HuAII/LCAT和HuLCAT动物相比,HuAI/LCAT和HuAI/AII/LCAT小鼠的HDL颗粒主要更大。与HuAI和HuAI/AII转基因小鼠相比,HuAI/LCAT和HuAI/AII/LCAT小鼠中LCAT活性的增加分别与前β-HDL组分中Hu载脂蛋白AI比例降低62%和27%相关。这些数据表明,LCAT活性的适度增加与脂蛋白胆固醇水平的显著变化有关,并且Hu LCAT对含有Hu载脂蛋白AI的HDL具有显著偏好。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/82e1/185767/da2235ccb979/jcinvest00015-0270-a.jpg

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