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小窝蛋白-1的表达是小窝蛋白-2转运至质膜所必需的。小窝蛋白-2滞留于高尔基体水平。

Expression of caveolin-1 is required for the transport of caveolin-2 to the plasma membrane. Retention of caveolin-2 at the level of the golgi complex.

作者信息

Parolini I, Sargiacomo M, Galbiati F, Rizzo G, Grignani F, Engelman J A, Okamoto T, Ikezu T, Scherer P E, Mora R, Rodriguez-Boulan E, Peschle C, Lisanti M P

机构信息

Department of Molecular Pharmacology, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

J Biol Chem. 1999 Sep 3;274(36):25718-25. doi: 10.1074/jbc.274.36.25718.

Abstract

Caveolins-1 and -2 are normally co-expressed, and they form a hetero-oligomeric complex in many cell types. These caveolin hetero-oligomers are thought to represent the assembly units that drive caveolae formation in vivo. However, the functional significance of the interaction between caveolins-1 and -2 remains unknown. Here, we show that caveolin-1 co-expression is required for the transport of caveolin-2 from the Golgi complex to the plasma membrane. We identified a human erythroleukemic cell line, K562, that expresses caveolin-2 but fails to express detectable levels of caveolin-1. This allowed us to stringently assess the effects of recombinant caveolin-1 expression on the behavior of endogenous caveolin-2. We show that expression of caveolin-1 in K562 cells is sufficient to reconstitute the de novo formation of caveolae in these cells. In addition, recombinant expression of caveolin-1 allows caveolin-2 to form high molecular mass oligomers that are targeted to caveolae-enriched membrane fractions. In striking contrast, in the absence of caveolin-1 expression, caveolin-2 forms low molecular mass oligomers that are retained at the level of the Golgi complex. Interestingly, we also show that expression of caveolin-1 in K562 cells dramatically up-regulates the expression of endogenous caveolin-2. Northern blot analysis reveals that caveolin-2 mRNA levels remain constant under these conditions, suggesting that the expression of caveolin-1 stabilizes the caveolin-2 protein. Conversely, transient expression of caveolin-2 in CHO cells is sufficient to up-regulate endogenous caveolin-1 expression. Thus, the formation of a hetero-oligomeric complex between caveolins-1 and -2 stabilizes the caveolin-2 protein product and allows caveolin-2 to be transported from the Golgi complex to the plasma membrane.

摘要

小窝蛋白-1和-2通常共同表达,并且它们在许多细胞类型中形成异源寡聚体复合物。这些小窝蛋白异源寡聚体被认为代表了在体内驱动小窝形成的组装单元。然而,小窝蛋白-1和-2之间相互作用的功能意义仍然未知。在这里,我们表明小窝蛋白-1的共同表达是小窝蛋白-2从高尔基体复合体转运到质膜所必需的。我们鉴定出一种人红白血病细胞系K562,它表达小窝蛋白-2但未能表达可检测水平的小窝蛋白-1。这使我们能够严格评估重组小窝蛋白-1表达对内源小窝蛋白-2行为的影响。我们表明在K562细胞中表达小窝蛋白-1足以在这些细胞中重新构建小窝的从头形成。此外,小窝蛋白-1的重组表达使小窝蛋白-2形成靶向富含小窝的膜组分的高分子量寡聚体。与之形成鲜明对比的是,在缺乏小窝蛋白-1表达的情况下,小窝蛋白-2形成低分子量寡聚体,这些寡聚体保留在高尔基体复合体水平。有趣的是,我们还表明在K562细胞中表达小窝蛋白-1显著上调内源小窝蛋白-2的表达。Northern印迹分析显示在这些条件下小窝蛋白-2的mRNA水平保持恒定,这表明小窝蛋白-1的表达稳定了小窝蛋白-2蛋白。相反,在CHO细胞中瞬时表达小窝蛋白-2足以上调内源小窝蛋白-1的表达。因此,小窝蛋白-1和-2之间异源寡聚体复合物的形成稳定了小窝蛋白-2蛋白产物,并使小窝蛋白-2能够从高尔基体复合体转运到质膜。

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