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Homeostasis of free cholesterol in the blood: a preliminary evaluation and modeling of its passive transport

机译:血液中游离胆固醇的体内平衡:其被动转运的初步评估和建模

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摘要

The rate of noncatalyzed transfer of cholesterol (Chol) among lipoproteins and cells in the blood is of fundamental importance as a baseline to assess the role of active transport mechanisms, but remains unknown. Here we address this gap by characterizing the associa­tion of the Chol analog, ergosta-5,7,9(11),22-tetraen-3β-ol (DHE), with the lipoproteins VLDL, LDL, HDL2, and HDL3. Combining these results with data for the association of DHE with liposomes, we elaborated a kinetic model for the noncatalyzed exchange of free Chol among blood compartments. The computational results are in good agreement with experimental values. The small deviations are explained by the nonequilibrium distribution of unesterified Chol in vivo, due to esterification and entry of new unesterified Chol, and eventual effects introduced by incubations at low temperatures. The kinetic profile of the homeostasis of unesterified Chol in the blood predicted by the model developed in this work is in good agreement with the observations in vivo, highlighting the importance of passive processes.
机译:血液中脂蛋白和细胞之间胆固醇(Chol)的非催化转移速率作为评估主动转运机制作用的基准具有根本的重要性,但仍未知。在这里,我们通过表征Chol类似物ergosta-5,7,9(11),22-tetraen-3β-ol(DHE)与脂蛋白VLDL,LDL,HDL2和HDL3的关联来解决这一差距。将这些结果与DHE与脂质体的关联数据结合起来,我们阐述了动力学模型用于血室之间游离Chol的非催化交换。计算结果与实验值吻合良好。小偏差可以通过未酯化的Chol在体内的不平衡分布来解释,这是由于酯化作用和新的未酯化的Chol的进入,以及在低温下孵育最终引入的影响所致。通过这项工作开发的模型预测的血液中未酯化Chol稳态的动力学特性与体内观察结果非常吻合,从而突出了被动过程的重要性。

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