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载脂蛋白脂肪酶 S447X 变异与代谢综合征中 VLDL、LDL 和 HDL 直径聚集相关。

Lipoprotein lipase S447X variant associated with VLDL, LDL and HDL diameter clustering in the MetS.

机构信息

Department of Epidemiology, University of Alabama at Birmingham, School of Public Health, Alabama, USA.

出版信息

Lipids Health Dis. 2011 Aug 19;10:143. doi: 10.1186/1476-511X-10-143.

Abstract

BACKGROUND

Previous analysis clustered 1,238 individuals from the general population Genetics of Lipid Lowering Drugs Network (GOLDN) study by the size of their fasting very low-density, low-density and high-density lipoproteins (VLDL, LDL, HDL) using latent class analysis. From two of the eight identified groups (N = 251), ~75% of individuals met Adult Treatment Panel III criteria for the metabolic syndrome (MetS). Both showed small LDL diameter (mean = 19.9 nm); however, group 1 (N = 200) had medium VLDL diameter (mean = 53.1 nm) while group 2 had very large VLDL diameter (mean = 65.74 nm). Group 2 additionally showed significantly more insulin resistance (IR), and accompanying higher waist circumference and fasting glucose and triglycerides (all P < .01). Since lipoprotein lipase hydrolyzes triglyceride in the VLDL-LDL cascade, we examined whether these two patterns of lipoprotein diameter were associated with differences across two lipoprotein lipase (LPL) gene variants: D9N (rs1801177) and S447X (rs328).

FINDINGS

Mixed linear models that controlled for age, sex, center of data collection, and family pedigree revealed no differences between the two groups for the D9N polymorphism (P = .36). However, group 2 contained significantly more carriers (25%) of the 447X variant than group 1 (14%; P = .04).

CONCLUSIONS

This was the first study this kind to show an association between LPL and large VLDL particle size within the MetS, a pattern associated with higher IR. Future work should extend this to larger samples to confirm these findings, and examine the long term outcomes of those with this lipoprotein diameter pattern.

摘要

背景

先前的分析使用潜在类别分析,根据空腹极低密度脂蛋白、低密度脂蛋白和高密度脂蛋白(VLDL、LDL、HDL)的大小,对来自一般人群脂质降低药物网络(GOLDN)研究的 1238 个人进行聚类。在确定的 8 个组中的 2 个(N=251)中,约 75%的个体符合成人治疗小组 III 代谢综合征(MetS)标准。两组的 LDL 直径均较小(均值=19.9nm);然而,第 1 组(N=200)的 VLDL 直径中等(均值=53.1nm),而第 2 组的 VLDL 直径非常大(均值=65.74nm)。第 2 组还显示出明显更高的胰岛素抵抗(IR),以及伴随的更高腰围、空腹血糖和甘油三酯(均 P<.01)。由于脂蛋白脂肪酶在 VLDL-LDL 级联中水解甘油三酯,我们检查了这两种脂蛋白直径模式是否与两种脂蛋白脂肪酶(LPL)基因变体的差异有关:D9N(rs1801177)和 S447X(rs328)。

发现

控制年龄、性别、数据收集中心和家族谱系的混合线性模型显示,两组之间 D9N 多态性没有差异(P=0.36)。然而,第 2 组携带 447X 变体的比例(25%)明显高于第 1 组(14%;P=0.04)。

结论

这是第一项研究表明,LPL 与 MetS 中较大的 VLDL 颗粒大小之间存在关联,这种模式与更高的 IR 相关。未来的工作应该扩大到更大的样本量来证实这些发现,并检查那些具有这种脂蛋白直径模式的人的长期结果。

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