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高α脂蛋白血症与前列腺素I2稳定性

Hyperalphalipoproteinemia and prostaglandin I2 stability.

作者信息

Pirich C, Efthimiou Y, O'Grady J, Sinzinger H

机构信息

Wilhelm Auerswald Atherosclerosis Research Group (ASF) Vienna, Austria.

出版信息

Thromb Res. 1997 Oct 1;88(1):41-9. doi: 10.1016/s0049-3848(97)00189-8.

DOI:10.1016/s0049-3848(97)00189-8
PMID:9336872
Abstract

PGI2 is a powerful regulator of thromboresistance modulating the local platelet/vessel wall interaction. Beside the amount synthesised the availability of the biologically active compound depends on its half-life at the site of action. Plasmatic half-life of PGI2 is extremely shortened during severe infections, but also in acute myocardial infarction with extremely lowered levels of HDL-c and apoAI, the latter being described as a potential PGI2-stabilising factor. These conditions are characterised by an enhanced thrombophilic risk. This study investigated for the first time whether high levels of HDL-c (mean: 95 +/- 13 mg/dl) and apoAI (mean: 179 +/- 13 mg/dl) which have been shown epidemiologically to protect against coronary heart disease in turn might be associated with an increase in PGI2 half-life. Results were obtained from 31 healthy subjects with hyperalpha-LP as compared with 10 controls. The biological half-life of PGI2 (hyperalpha-LP: mean: 915 +/- 118 sec vs. controls: 714 +/- 70 sec; p = 0.001) was positively related to HDL-c (r = 0.8795, p < 0.001) and apoAI levels (r = 0.8025, p < 0.001). The partial correlation coefficient correcting for the association between HDL-c and apoAI levels was also significant (PGI2 to HDL-c: r = 0.6000, p < 0.001). These results suggest that the antiatherosclerotic properties of HDL might be at least partly due to an increase in PGI2 half-life.

摘要

前列环素(PGI2)是血栓抗性的强大调节剂,可调节局部血小板与血管壁的相互作用。除了合成量外,生物活性化合物的可用性还取决于其在作用部位的半衰期。在严重感染期间,PGI2的血浆半衰期会极短缩短,在急性心肌梗死中,当高密度脂蛋白胆固醇(HDL-c)和载脂蛋白AI(apoAI)水平极低时也会如此,后者被认为是一种潜在的PGI2稳定因子。这些情况的特征是血栓形成风险增加。本研究首次调查了流行病学研究显示可预防冠心病的高水平HDL-c(平均:95±13mg/dl)和apoAI(平均:179±13mg/dl)是否反过来可能与PGI2半衰期的延长有关。研究结果来自31名高α脂蛋白血症的健康受试者,并与10名对照者进行比较。PGI2的生物半衰期(高α脂蛋白血症组:平均:915±118秒,对照组:714±70秒;p = 0.001)与HDL-c(r = 0.8795,p < 0.001)和apoAI水平(r = 0.8025,p < 0.001)呈正相关。校正HDL-c和apoAI水平之间关联后的偏相关系数也具有显著性(PGI2与HDL-c:r = 0.6000,p < 0.001)。这些结果表明,HDL的抗动脉粥样硬化特性可能至少部分归因于PGI2半衰期的延长。

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