首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Metabolism of apolipoprotein B in large triglyceride-rich very low density lipoproteins of normal and hypertriglyceridemic subjects.
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Metabolism of apolipoprotein B in large triglyceride-rich very low density lipoproteins of normal and hypertriglyceridemic subjects.

机译:正常和高甘油三酸酯血症受试者中富含甘油三酸酯的超低密度脂蛋白中载脂蛋白B的代谢。

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摘要

The metabolic fate of very low density lipoprotein can be examined by following the transit of its apolipoprotein B moiety through the delipidation cascade, which leads to low density lipoprotein. In this study we have used cumulative flotation ultracentrifugation to follow the metabolism of various lipoprotein subclasses that participate in this process in normal, hypertriglyceridemic (Type IV), and dysbetalipoproteinemic (Type III) subjects. Large triglyceride-rich very low density lipoproteins of Svedberg units of flotation (Sf) 100-400 were converted virtually quantitatively in normal subjects to smaller Sf 12-100 remnant particles. Only a minor fraction appeared thereafter in low density lipoproteins (Sf 0-12), most being removed directly from the plasma. Type IV hyperlipoproteinemic individuals converted the larger Sf 100-400 very low density lipoproteins to intermediate particles at approximately 50% of the control rate but thereafter their metabolism was normal (fractional clearance of Sf 12-100 particles in controls, 1.29 +/- 0.23 pools/d; in Type IV hypertriglyceridemics, 1.38 +/- 0.23 pools/d; n = 4 in each case). Since the apolipoprotein B in large triglyceride-rich particles did not contribute significantly to the mass of the low density lipoprotein apoprotein pool, the latter must come largely from another source. This was examined by following the metabolic fate of small very low density lipoproteins of Sf 20-60 or of the total lipoprotein spectrum of d less than 1.006 kg/liter (approximate Sf 20-400). The small particles were rapidly and substantially converted to low density lipoproteins, suggesting that the major precursor of the latter was to be found in this density range. Whereas only 10% of apolipoprotein B in Sf 100-400 lipoproteins reached the low density lipoprotein flotation range, greater than 40% of Sf 20-100 B protein eventually appeared in Sf 0-12 particles; and when very low density lipoprotein of d less than 1.006 kg/liter is used as a tracer of apolipoprotein B metabolism it is primarily this population of small very low density lipoprotein particles in the Sf 12-100 flotation range that is labeled. A detailed examination was made of apolipoprotein B metabolism in three dysbetalipoproteinemic subjects. The plasma clearance curves of their Sf 100-400 lipoproteins were distinctly biphasic. The quickly decaying component converted rapidly into remnants of Sf 20-60 at a near normal rate (0.56 vs. 0.62 pools/d in normal subjects). Its subsequent processing, however, was retarded. The more slowly catabolized fraction, comprising 30% of the total apolipoprotein B radioactivity, had no counterpart in normal or Type IV hyperlipoproteinemic individuals. These data, taken together, suggest that the very low density lipoprotein consists of a complex mixture of particles with different origins and fates. Within the Sf 20-100 flotation range there are at least two subcomponents. One represents remnants of larger triglyceride-rich particles which are catabolized slowly and feeds little apolipoprotein B into low density lipoprotein. The other is apparently secreted directly into this flotation interval and transfers significant amounts of B protein rapidly into Sf 0-12 lipoproteins.
机译:可以通过追踪其载脂蛋白B部分穿过脂质级联反应来检测极低密度脂蛋白的代谢命运,从而导致低密度脂蛋白。在这项研究中,我们已使用累积浮选超速离心法来跟踪正常,高甘油三酸酯血症(IV型)和高脂蛋白脂蛋白异常(III型)受试者参与该过程的各种脂蛋白亚类的代谢。 Svedberg浮选单位(Sf)100-400中富含甘油三酸酯的极低密度大型脂蛋白实际上在正常受试者中定量地转化为较小的Sf 12-100残留颗粒。此后,在低密度脂蛋白(Sf 0-12)中仅出现一小部分,大部分直接从血浆中去除。 IV型高脂蛋白血症个体以约50%的控制率将较大的Sf 100-400非常低密度脂蛋白转化为中间颗粒,但随后其代谢正常(对照组中Sf 12-100颗粒的部分清除率为1.29 +/- 0.23池) / d;在IV型高甘油三酯血症患者中,每天1.38 +/- 0.23池/ d;在每种情况下,n = 4)。由于富含甘油三酸酯的大颗粒中的载脂蛋白B对低密度脂蛋白载脂蛋白库的质量没有显着贡献,因此后者必须主要来自其他来源。通过追踪Sf 20-60的极低密度小脂蛋白或d的总脂蛋白谱小于1.006 kg / L(约Sf 20-400)的代谢命运来检验这一点。小颗粒迅速并基本转化为低密度脂蛋白,表明后者的主要前体在此密度范围内。 Sf 100-400脂蛋白中只有10%的载脂蛋白B达到低密度脂蛋白浮选范围,而Sf 0-12颗粒中最终出现了超过40%的Sf 20-100 B蛋白;当使用小于1.006千克/升的d极低密度脂蛋白作为载脂蛋白B代谢的示踪剂时,主要是在Sf 12-100浮选范围内标记了该极小的低密度脂蛋白小颗粒群。在三个脂蛋白脂蛋白异常的受试者中对载脂蛋白B代谢进行了详细检查。他们的Sf 100-400脂蛋白的血浆清除率曲线明显是两相的。快速衰变的成分以接近正常的速率迅速转化为Sf 20-60的残留物(正常受试者中0.56比0.62库/ d)。然而,其随后的处理受到阻碍。分解代谢较慢的部分占载脂蛋白B放射性总量的30%,在正常或IV型高脂蛋白血症个体中没有对应物。这些数据加在一起表明,极低密度脂蛋白由具有不同起源和命运的颗粒的复杂混合物组成。在Sf 20-100浮选范围内,至少有两个子组件。一个代表较大的富含甘油三酸酯的颗粒的残留物,这些颗粒缓慢分解代谢,几乎没有载脂蛋白B进入低密度脂蛋白。另一个显然是直接分泌到该浮选区间中,并将大量B蛋白迅速转移到Sf 0-12脂蛋白中。

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