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载脂蛋白定义的脂蛋白家族概念及其临床意义。

The concept of apolipoprotein-defined lipoprotein families and its clinical significance.

作者信息

Alaupovic Petar

机构信息

Lipid and Lipoprotein Laboratory, Oklahoma Medical Research Foundation, 800 Research Parkway, Suite 340, Oklahoma City, OK 73104, USA.

出版信息

Curr Atheroscler Rep. 2003 Nov;5(6):459-67. doi: 10.1007/s11883-003-0036-8.

Abstract

Classification of plasma lipoproteins on the basis of apolipoprotein (apo) composition recognizes two lipoprotein (Lp) classes, one of which is characterized by apoA-I and the other by apoB as major protein constituents. The former lipoprotein class consists of three major subclasses referred to (according to their apolipoprotein constituents) as Lp-A-I, Lp-A-I:A-II, and Lp-A-II, and the latter one of five subclasses called Lp-B, Lp-B:E, Lp-B:C, Lp-B:C:E, and Lp-A-II:B:C:D:E. As polydisperse systems of particles, the apoA-I-containing lipoproteins overlap in high-density segments and apoB- containing lipoproteins in low-density segments of the density gradient. Each subclass is characterized by a specific chemical composition and metabolic property. Normolipidemia and dyslipoproteinemias are characterized by quantitative rather than qualitative differences in the levels of apoA- and apoB-containing subclasses. Furthermore, apoA-containing subclasses seem to differ with respect to their relative antiatherogenic capacities, and apoB-containing subclasses regarding their relative atherogenic potentials. Whereas Lp-A-I may have a greater antiatherogenic capacity than other apoA-containing subclasses, the cholesterol-enriched Lp-B:C appears to be the most atherogenic subclass among apoB-containing lipoprotein families. The use of pharmacologic and/or dietary interventions to treat dyslipoproteinemias has already shown that these therapeutic modalities may affect selectively individual apolipoprotein-defined lipoproteins, and thus allow the selection of individualized treatments targeted at decreasing harmful and/or increasing beneficial lipoprotein subclasses.

摘要

基于载脂蛋白(apo)组成对血浆脂蛋白进行分类可识别出两类脂蛋白(Lp),其中一类以apoA-I为特征,另一类以apoB作为主要蛋白质成分。前一类脂蛋白由三个主要亚类组成(根据其载脂蛋白成分),分别称为Lp-A-I、Lp-A-I:A-II和Lp-A-II,后一类由五个亚类组成,称为Lp-B、Lp-B:E、Lp-B:C、Lp-B:C:E和Lp-A-II:B:C:D:E。作为多分散的颗粒系统,含apoA-I的脂蛋白在密度梯度的高密度段重叠,含apoB的脂蛋白在低密度段重叠。每个亚类都具有特定的化学组成和代谢特性。正常血脂血症和血脂异常血症的特征在于含apoA和apoB的亚类水平的定量差异而非定性差异。此外,含apoA的亚类在其相对抗动脉粥样硬化能力方面似乎有所不同,含apoB的亚类在其相对动脉粥样硬化潜力方面也有所不同。虽然Lp-A-I可能比其他含apoA的亚类具有更大的抗动脉粥样硬化能力,但富含胆固醇的Lp-B:C似乎是含apoB的脂蛋白家族中最具动脉粥样硬化性的亚类。使用药物和/或饮食干预来治疗血脂异常血症已经表明,这些治疗方式可能会选择性地影响个别载脂蛋白定义的脂蛋白,从而允许选择针对减少有害和/或增加有益脂蛋白亚类的个体化治疗方法。

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