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高密度脂蛋白介导的胆固醇摄取及在完整L细胞成纤维细胞中靶向脂滴的研究。单光子和多光子荧光方法。

High density lipoprotein-mediated cholesterol uptake and targeting to lipid droplets in intact L-cell fibroblasts. A single- and multiphoton fluorescence approach.

作者信息

Frolov A, Petrescu A, Atshaves B P, So P T, Gratton E, Serrero G, Schroeder F

机构信息

Department of Pathobiology, Texas A & M University, Texas Veterinary Medical Center, College Station, Texas 77843-4466, USA.

出版信息

J Biol Chem. 2000 Apr 28;275(17):12769-80. doi: 10.1074/jbc.275.17.12769.

DOI:10.1074/jbc.275.17.12769
PMID:10777574
Abstract

Fluorescent sterols, dehydroergosterol and NBD-cholesterol, were used to examine high density lipoprotein-mediated cholesterol uptake and intracellular targeting in L-cell fibroblasts. The uptake, but not esterification or targeting to lipid droplets, of these sterols differed >100-fold, suggesting significant differences in uptake pathways. NBD-cholesterol uptake kinetics and lipoprotein specificity reflected high density lipoprotein-mediated sterol uptake via the scavenger receptor B1. Fluorescence energy transfer showed an average intermolecular distance of 26 A between the two fluorescent sterols in L-cells. Indirect immunofluorescence revealed that both fluorescent sterols localized to L-cell lipid droplets, the surface of which contained adipose differentiation-related protein. This lipid droplet-specific protein specifically bound NBD-cholesterol with high affinity (K(d) = 2 nM) at a single site. Thus, NBD-cholesterol and dehydroergosterol were useful fluorescent probes of sterol uptake and intracellular sterol targeting. NBD-cholesterol more selectively probed high density lipoprotein-mediated uptake and rapid intracellular targeting of sterol to lipid droplets. Targeting of sterol to lipid droplets was correlated with the presence of adipose differentiation related protein, a lipid droplet-specific protein shown for the first time to bind unesterified sterol with high affinity.

摘要

荧光固醇、脱氢麦角固醇和NBD-胆固醇被用于研究高密度脂蛋白介导的胆固醇摄取以及L细胞成纤维细胞中的细胞内靶向作用。这些固醇的摄取情况(而非酯化或靶向脂滴的情况)相差超过100倍,这表明摄取途径存在显著差异。NBD-胆固醇的摄取动力学和脂蛋白特异性反映了通过清道夫受体B1介导的高密度脂蛋白固醇摄取。荧光能量转移显示L细胞中两种荧光固醇之间的平均分子间距离为26埃。间接免疫荧光显示两种荧光固醇都定位于L细胞脂滴,其表面含有脂肪分化相关蛋白。这种脂滴特异性蛋白在单个位点以高亲和力(K(d)=2 nM)特异性结合NBD-胆固醇。因此,NBD-胆固醇和脱氢麦角固醇是固醇摄取和细胞内固醇靶向作用的有用荧光探针。NBD-胆固醇更有选择性地探测了高密度脂蛋白介导的固醇摄取以及固醇向脂滴的快速细胞内靶向作用。固醇向脂滴的靶向作用与脂肪分化相关蛋白的存在相关,脂肪分化相关蛋白是一种脂滴特异性蛋白,首次被证明能以高亲和力结合未酯化的固醇。

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