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Noninvasive Neutron Scattering Measurements Reveal Slower Cholesterol Transport in Model Lipid Membranes

机译:非侵入性中子散射测量揭示了模型脂质膜中较慢的胆固醇转运。

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摘要

Proper cholesterol transport is essential to healthy cellular activity and any abnormality can lead to several fatal diseases. However, complete understandings of cholesterol homeostasis in the cell remains elusive, partly due to the wide variability in reported values for intra- and intermembrane cholesterol transport rates. Here, we used time-resolved small-angle neutron scattering to measure cholesterol intermembrane exchange and intramembrane flipping rates, in situ, without recourse to any external fields or compounds. We found significantly slower transport kinetics than reported by previous studies, particularly for intramembrane flipping where our measured rates are several orders of magnitude slower. We unambiguously demonstrate that the presence of chemical tags and extraneous compounds employed in traditional kinetic measurements dramatically affect the system thermodynamics, accelerating cholesterol transport rates by an order of magnitude. To our knowledge, this work provides new insights into cholesterol transport process disorders, and challenges many of the underlying assumptions used in most cholesterol transport studies to date.
机译:正确的胆固醇转运对于健康的细胞活动至关重要,任何异常都会导致几种致命的疾病。但是,对细胞内胆固醇稳态的完整了解仍然难以捉摸,部分原因是膜内和膜间胆固醇转运速率的报道值存在很大差异。在这里,我们使用时间分辨小角度中子散射来原位测量胆固醇的膜交换和膜内翻转速率,而无需求助于任何外部场或化合物。我们发现运输动力学明显比以前的研究报告慢,尤其是对于膜内翻转,我们的测量速率要慢几个数量级。我们毫不含糊地证明,传统动力学测量中使用的化学标签和外来化合物的存在会显着影响系统的热力学,从而将胆固醇的传输速率提高一个数量级。据我们所知,这项工作提供了有关胆固醇转运过程疾病的新见解,并挑战了迄今为止大多数胆固醇转运研究中使用的许多基本假设。

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