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利用点击化学追踪 20(s)-羟基胆固醇的亚细胞命运,揭示了一条通向高尔基体的运输途径。

Tracking the subcellular fate of 20(s)-hydroxycholesterol with click chemistry reveals a transport pathway to the Golgi.

机构信息

Departments of Medicine and Stanford University School of Medicine, Stanford, California 94305.

Biochemistry, Stanford University School of Medicine, Stanford, California 94305, and.

出版信息

J Biol Chem. 2014 Apr 18;289(16):11095-11110. doi: 10.1074/jbc.M113.540351. Epub 2014 Mar 4.

Abstract

Oxysterols, oxidized metabolites of cholesterol, are endogenous small molecules that regulate lipid metabolism, immune function, and developmental signaling. Although the cell biology of cholesterol has been intensively studied, fundamental questions about oxysterols, such as their subcellular distribution and trafficking pathways, remain unanswered. We have therefore developed a useful method to image intracellular 20(S)-hydroxycholesterol with both high sensitivity and spatial resolution using click chemistry and fluorescence microscopy. The metabolic labeling of cells with an alkynyl derivative of 20(S)-hydroxycholesterol has allowed us to directly visualize this oxysterol by attaching an azide fluorophore through cyclo-addition. Unexpectedly, we found that this oxysterol selectively accumulates in the Golgi membrane using a pathway that is sensitive to ATP levels, temperature, and lysosome function. Although previous models have proposed nonvesicular pathways for the rapid equilibration of oxysterols between membranes, direct imaging of oxysterols suggests that a vesicular pathway is responsible for differential accumulation of oxysterols in organelle membranes. More broadly, clickable alkynyl sterols may represent useful tools for sterol cell biology, both to investigate the functions of these important lipids and to decipher the pathways that determine their cellular itineraries.

摘要

氧化固醇是胆固醇的氧化代谢物,是内源性小分子,可调节脂代谢、免疫功能和发育信号。尽管胆固醇的细胞生物学已得到深入研究,但氧化固醇的一些基本问题,如它们的亚细胞分布和运输途径,仍未得到解答。因此,我们开发了一种有用的方法,利用点击化学和荧光显微镜,以高灵敏度和空间分辨率对细胞内 20(S)-羟基胆固醇进行成像。通过用炔基衍生物对细胞进行代谢标记,我们可以通过环加成将叠氮荧光团连接到该氧化固醇上来直接可视化它。出乎意料的是,我们发现这种氧化固醇选择性地积累在高尔基体膜中,该途径对 ATP 水平、温度和溶酶体功能敏感。虽然以前的模型提出了非囊泡途径来快速平衡膜之间的氧化固醇,但氧化固醇的直接成像表明囊泡途径负责氧化固醇在细胞器膜中差异积累。更广泛地说,可点击的炔基固醇可能是固醇细胞生物学的有用工具,既可以研究这些重要脂质的功能,也可以解析决定它们细胞途径的途径。

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