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首页> 外文期刊>Clinical Chemistry: Journal of the American Association for Clinical Chemists >Evaluation of the dual-precipitation method for determination of cholesterol in high-density lipoprotein subfractions HDL2 and HDL3 in serum.
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Evaluation of the dual-precipitation method for determination of cholesterol in high-density lipoprotein subfractions HDL2 and HDL3 in serum.

机译:测定血清中高密度脂蛋白亚组分HDL2和HDL3中胆固醇的双重沉淀方法的评估。

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We compared the dual-precipitation method for measurement of cholesterol in high-density lipoprotein subfractions HDL2 and HDL3 (Gidez et al., J Lipid Res 1982;23:1206-33) with density-gradient ultracentrifugation in a swinging-bucket rotor (Demacker et al., Clin Chem 1983;29:656-63). The concentration of dextran sulfate 15,000 (DS) needed for optimal accuracy of the HDL2-chol and HDL3-chol values was established empirically. At a DS concentration of 0.87 g/L, the values for HDL2-chol as well as for HDL3-chol in 88 sera did not differ significantly from those obtained by ultracentrifugation. The precision of the method was satisfactory and was related to the concentration. Nevertheless, the dual-precipitation method lacks specificity inasmuch as it produces no fractions that contain only one HDL subfraction. HDL2 and HDL3 each contained an equivalent amount of cholesterol from the other. At increasing DS concentrations, some radiolabeled HDL3 appeared to have precipitated prior to complete precipitation of HDL2. This lack of specificity can be tolerated in large-scale epidemiological studies for screening, but not in small-scale intervention studies or in assay of clinical samples, where better accuracy is needed and ultracentrifugation is preferred.
机译:我们将在高密度脂蛋白亚组分HDL2和HDL3(Gidez等,J Lipid Res 1982; 23:1206-33)中使用胆固醇的双沉淀法与密度梯度超速离心斗式转子(Demacker)中的胆固醇进行了比较等人,Clin Chem 1983; 29:656-63)。根据经验确定了HDL2-chol和HDL3-chol值的最佳准确度所需的硫酸葡聚糖15,000(DS)的浓度。在DS浓度为0.87 g / L时,88血清中HDL2-chol和HDL3-chol的值与超速离心获得的值没有显着差异。该方法的精密度令人满意,并且与浓度有关。然而,双重沉淀法缺乏特异性,因为它不产生仅包含一个HDL亚馏分的馏分。 HDL2和HDL3各自含有等量的胆固醇。在DS浓度增加时,一些放射性标记的HDL3似乎在HDL2完全沉淀之前已经沉淀。这种缺乏特异性可以在大规模的流行病学研究中进行筛查,但在小规模的干预研究或临床样品的测定中则无法忍受,因为在这种情况下,需要更高的准确性,并且首选超速离心。

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