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脂蛋白胆固醇组分的多变量分析。

Multivariate analysis of lipoprotein cholesterol fractions.

作者信息

Vogler G P, Rao D C, Laskarzewski P M, Glueck C J, Russell J M

出版信息

Am J Epidemiol. 1987 Apr;125(4):706-19. doi: 10.1093/oxfordjournals.aje.a114583.

Abstract

Intervention and prevention of multifactorial diseases such as coronary heart disease can be effective only when the joint effects of multiple risk factors are known. This process is facilitated by multivariate analysis of correlated risk factors, such as the serum cholesterol fractions, high density lipoprotein (HDL), low density lipoprotein (LDL), and very low density lipoprotein (VLDL). Whereas evidence for genetic covariation provides focus for further refined biochemical analysis, covariation among environmental factors can point to efficacious intervention strategies. To assess sources of variation and covariation among HDL, LDL, and VLDL, a multivariate path model was developed and applied to family data. Phenotypic variance is due primarily to specific environmental influences with substantial genetic influences, with the common family environment contributing less than 10% of the variance. There are genetic correlations of -0.22 for HDL-VLDL and 0.35 for VLDL-LDL, consistent with the known inverse associations of HDL and VLDL and the precursor-product relationship between VLDL and LDL, whereas there is no evidence for a direct HDL-LDL genetic relationship. Strong specific environmental correlations are found between HDL and VLDL (-0.35 in children and -0.50 in adults). Thus, intervention focused primarily on one fraction (e.g., triglycerides and VLDL) might beneficially affect levels of both lipoproteins (e.g., lowering VLDL cholesterol and elevating HDL cholesterol). Multivariate analysis can facilitate understanding of the linked effects of intervention on lipoprotein cholesterols, and, hence, should benefit approaches to maximize the effects of lipoprotein cholesterol intervention on coronary heart disease morbidity and mortality.

摘要

只有在了解多种风险因素的联合作用时,对冠心病等多因素疾病的干预和预防才会有效。对相关风险因素进行多变量分析有助于这一过程,比如血清胆固醇组分、高密度脂蛋白(HDL)、低密度脂蛋白(LDL)和极低密度脂蛋白(VLDL)。虽然基因共变的证据为进一步精细的生化分析提供了重点,但环境因素之间的共变可以指向有效的干预策略。为了评估HDL、LDL和VLDL之间变异和共变的来源,开发了一个多变量路径模型并将其应用于家庭数据。表型变异主要归因于特定环境影响和显著的基因影响,共同家庭环境对变异的贡献不到10%。HDL与VLDL的基因相关性为-0.22,VLDL与LDL的基因相关性为0.35,这与HDL和VLDL之间已知的负相关以及VLDL和LDL之间的前体-产物关系一致,而没有证据表明HDL与LDL之间存在直接的基因关系。在HDL和VLDL之间发现了很强的特定环境相关性(儿童中为-0.35,成人中为-0.50)。因此,主要针对一个组分(如甘油三酯和VLDL)的干预可能会对两种脂蛋白的水平产生有益影响(如降低VLDL胆固醇并升高HDL胆固醇)。多变量分析有助于理解干预对脂蛋白胆固醇的连锁效应,因此,应该有利于最大化脂蛋白胆固醇干预对冠心病发病率和死亡率影响的方法。

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