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首页> 外文期刊>Journal of Lipid Research >A novel approach to measuring macrophage-specific reverse cholesterol transport in vivo in humans
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A novel approach to measuring macrophage-specific reverse cholesterol transport in vivo in humans

机译:一种新的人类体内巨噬细胞特异性反向胆固醇转运的新方法

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摘要

Reverse cholesterol transport (RCT) is thought to be an atheroprotective function of HDL, and macrophage-specific RCT in mice is inversely associated with atherosclerosis. We developed a novel method using H-3-cholesterol nanoparticles to selectively trace macrophage-specific RCT in vivo in humans. Use of H-3-cholesterol nanoparticles was initially tested in mice to assess the distribution of tracer and response to interventions known to increase RCT. Thirty healthy subjects received H-3-cholesterol nanoparticles intravenously, followed by blood and stool sample collection. Tracer counts were assessed in plasma, nonHDL, HDL, and fecal fractions. Data were analyzed by using multicompartmental modeling. Administration of H-3-cholesterol nanoparticles preferentially labeled macrophages of the reticuloendothelial system in mice, and counts were increased in mice treated with a liver X receptor agonist or reconstituted HDL, as compared with controls. In humans, tracer disappeared from plasma rapidly after injection of nanoparticles, followed by reappearance in HDL and nonHDL fractions. Counts present as free cholesterol increased rapidly and linearly in the first 240 min after nadir; counts in cholesteryl ester increased steadily over time. Estimates of fractional transfer rates of key RCT steps were obtained. These results support the use of H-3-cholesterol nanoparticles as a feasible approach for the measurement of macrophage RCT in vivo in humans.
机译:反向胆固醇转运(RCT)被认为是HDL的动脉保护功能,小鼠中的巨噬细胞特异性RCT与动脉粥样硬化相反。我们开发了一种使用H-3-胆固醇纳米粒子的新方法,以在人体中选择性地追踪巨噬细胞特异性RCT。最初在小鼠中测试H-3-胆固醇纳米颗粒以评估示踪剂的分布和对已知RCT的干预措施的响应。 30个健康受试者静脉内接受H-3-胆固醇纳米粒子,然后是血液和粪便样品收集。在血浆,非向量,HDL和粪便级分中评估跟踪计数。通过使用多组分建模分析数据。施用H-3-胆固醇纳米颗粒优先标记在小鼠中的近噬细胞的巨噬细胞,与对照相比,用肝X受体激动剂或重构的HDL处理的小鼠中的计数增加。在人类中,在注射纳米颗粒后,示踪剂从血浆中从等离子体中消失,然后重新出现HDL和非加入级分。在Nadir之后的前240分钟内,作为游离胆固醇的计数迅速和线性迅速增加;随着时间的推移,胆固醇酯的计数稳定地增加。获得了关键RCT步骤的分数传递率的估计。这些结果支持使用H-​​3-胆固醇纳米颗粒作为用于测量人类体内巨噬细胞RCT的可行方法。

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