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膜脂与阴离子转运蛋白带3通过硫脲修饰的两亲性脂质探针在体内的连接

In Vivo Linking of Membrane Lipids and the Anion Transporter Band 3 with Thiourea-modified Amphiphilic Lipid Probes.

作者信息

Moriyama Akihiro, Katagiri Naohiro, Nishimura Shinichi, Takahashi Nobuaki, Kakeya Hideaki

机构信息

Department of System Chemotherapy and Molecular Sciences, Division of Bioinformatics and Chemical Genomics, Graduate School of Pharmaceutical Sciences, Kyoto University, Sakyo-ku, Kyoto 606-8501, Japan.

出版信息

Sci Rep. 2015 Nov 30;5:17427. doi: 10.1038/srep17427.

Abstract

Membrane proteins interact with membrane lipids for their structural stability and proper function. However, lipid-protein interactions are poorly understood at a molecular level especially in the live cell membrane, due to current limitations in methodology. Here, we report that amphiphilic lipid probes can be used to link membrane lipids and membrane proteins in vivo. Cholesterol and a phospholipid were both conjugated to a fluorescent tag through a linker containing thiourea. In the erythrocyte, the cholesterol probe fluorescently tagged the anion transporter band 3 via thiourea. Tagging by the cholesterol probe, but not by the phospholipid probe, was competitive with an anion transporter inhibitor, implying the presence of a specific binding pocket for cholesterol in this ~100 kDa protein. This method could prove an effective strategy for analyzing lipid-protein interactions in vivo in the live cell membrane.

摘要

膜蛋白与膜脂相互作用以维持其结构稳定性和正常功能。然而,由于目前方法学上的局限性,脂质-蛋白质相互作用在分子水平上,尤其是在活细胞膜中,仍了解甚少。在此,我们报告两亲性脂质探针可用于在体内连接膜脂和膜蛋白。胆固醇和一种磷脂都通过含硫脲的连接子与荧光标签偶联。在红细胞中,胆固醇探针通过硫脲对阴离子转运蛋白带3进行荧光标记。胆固醇探针而非磷脂探针的标记与阴离子转运抑制剂具有竞争性,这意味着在这种约100 kDa的蛋白质中存在胆固醇的特异性结合口袋。该方法可能是分析活细胞膜中体内脂质-蛋白质相互作用的有效策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a8a0/4663539/babbae381790/srep17427-f1.jpg

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