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Mouse hepatic lipase alleles with variable effects on lipoprotein composition and size

机译:小鼠肝脂肪酶等位基因对脂蛋白组成和大小的影响不同

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摘要

The structural features responsible for the activities of hepatic lipase (HL) can be clarified by in vivo comparisons of naturally occurring variants. The coding sequence of HL from C57BL/6J (B6) and SPRET/EiJ (SPRET) mice differs by four amino acids (S106N, A156V, L416V, S480T); however, these changes are not predicted to influence HL function. To test for allelic effects, we generated SPRET-HL transgenics with physiological levels of HL mRNA and HL activity that was parallel in female transgenics and about 70% higher in male transgenics, toward tri-[3H]oleate, compared with B6 controls. We found no correlation between activity levels and plasma lipids. However, significant allelic effects on plasma lipids were observed. Compared with B6-HL, SPRET-HL mediated reductions in total cholesterol (TC) and VLDL-, LDL- and HDL-cholesterol and HDL-triglyceride (TG) in fed males, and SPRET-HL decreased total TG and VLDL- and HDL-TG levels in fasted males. Fasted female transgenics had reduced TC compared with controls. We also found allele and sex effects on lipoprotein particle size. Male transgenic mice had increased VLDL and decreased LDL size, and female transgenic mice had decreased HDL size compared with control animals. These findings demonstrate highly divergent effects of naturally occurring HL coding sequence variants on lipid and lipoprotein metabolism.
机译:可以通过体内比较天然存在的变体来阐明负责肝脂肪酶(HL)活性的结构特征。来自C57BL / 6J(B6)和SPRET / EiJ(SPRET)小鼠的HL的编码序列相差四个氨基酸(S106N,A156V,L416V,S480T);然而,这些变化预计不会影响HL功能。为了测试等位基因效应,我们生成了SPRET-HL转基因,其生理水平的HL mRNA和HL活性与B6对照相比,在女性转基因中平行,在男性转基因中相对于[3H]油酸酯高70%。我们发现活性水平和血浆脂质之间没有相关性。然而,观察到对血浆脂质的显着等位基因作用。与B6-HL相比,SPRET-HL介导的饲喂雄性总胆固醇(TC)和VLDL-,LDL-和HDL-胆固醇和HDL-甘油三酸酯(TG)降低,而SPRET-HL降低了总TG和VLDL-和HDL -禁食男性的TG水平。与对照相比,禁食的女性转基因基因降低了TC。我们还发现等位基因和性别对脂蛋白粒径的影响。与对照动物相比,雄性转基因小鼠的VLDL增加,LDL大小减小,雌性转基因小鼠的HDL大小减小。这些发现证明了天然存在的HL编码序列变体对脂质和脂蛋白代谢的高度不同的影响。

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