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用糖鞘脂C8-β-D-乳糖神经酰胺处理成纤维细胞后,对转运至膜微区的蛋白质进行蛋白质组学鉴定。

Proteomic identification of proteins translocated to membrane microdomains upon treatment of fibroblasts with the glycosphingolipid, C8-beta-D-lactosylceramide.

作者信息

Kim Seong-Youl, Wang Teng-ke, Singh Raman Deep, Wheatley Christine L, Marks David L, Pagano Richard E

机构信息

Department of Biochemistry and Molecular Biology, Thoracic Diseases Research Unit, Mayo Clinic College of Medicine, Rochester, MN 55905-0001, USA.

出版信息

Proteomics. 2009 Sep;9(18):4321-8. doi: 10.1002/pmic.200900077.

Abstract

Plasma membrane (PM) microdomains, including caveolae and other cholesterol-enriched subcompartments, are involved in the regulation of many cellular processes, including endocytosis, attachment and signaling. We recently reported that brief incubation of human skin fibroblasts with the synthetic glycosphingolipid, D-erythro-octanoyl-lactosylceramide (C8-D-e-LacCer), stimulates endocytosis via caveolae and induces the appearance of micron-size microdomains on the PM. To further understand the effects of C8-D-e-LacCer treatment on PM microdomains, we used a detergent-free method to isolate microdomain-enriched membranes from fibroblasts treated +/-C8-D-e-LacCer, and performed 2-DE and mass spectrophotometry to identify proteins that were altered in their distribution in microdomains. Several proteins were identified in the microdomain-enriched fractions, including lipid transfer proteins and proteins related to the functions of small GTPases. One protein, Rho-associated protein kinase 2 (ROCK2), was verified by Western blotting to occur in microdomain fractions and to increase in these fractions after D-e-LacCer treatment. Immunofluorescence revealed that ROCK2 exhibited an increased localization at or near the PM in C8-D-e-LacCer-treated cells. In contrast, ROCK2 distribution in microdomains was decreased by treatment of cells with C8-L-threo-lactosylceramide, a glycosphingolipid with non-natural stereochemistry. This study identifies new microdomain-associated proteins and provides evidence that microdomains play a role in the regulation of the Rho/ROCK signaling pathway.

摘要

质膜(PM)微结构域,包括小窝和其他富含胆固醇的亚结构区,参与许多细胞过程的调节,包括内吞作用、细胞黏附和信号传导。我们最近报道,用人皮肤成纤维细胞与合成糖鞘脂D-赤藓糖辛酰乳糖神经酰胺(C8-D-e-LacCer)进行短暂孵育,可通过小窝刺激内吞作用,并在质膜上诱导微米大小微结构域的出现。为了进一步了解C8-D-e-LacCer处理对质膜微结构域的影响,我们采用无去污剂方法从经C8-D-e-LacCer处理或未处理的成纤维细胞中分离富含微结构域的膜,并进行二维电泳和质谱分析,以鉴定其在微结构域中分布发生改变的蛋白质。在富含微结构域的组分中鉴定出了几种蛋白质,包括脂质转运蛋白和与小GTP酶功能相关的蛋白质。一种蛋白质,即Rho相关蛋白激酶2(ROCK2),通过蛋白质免疫印迹法验证其存在于微结构域组分中,并且在D-e-LacCer处理后这些组分中含量增加。免疫荧光显示,在经C8-D-e-LacCer处理的细胞中,ROCK2在质膜处或其附近的定位增加。相反,用具有非天然立体化学结构的糖鞘脂C8-L-苏式乳糖神经酰胺处理细胞后,ROCK2在微结构域中的分布减少。本研究鉴定了新的与微结构域相关的蛋白质,并提供了证据表明微结构域在Rho/ROCK信号通路的调节中发挥作用。

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