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H-ras在质膜微结构域中的分布和信号传导受酰化和去酰化事件调控。

H-ras distribution and signaling in plasma membrane microdomains are regulated by acylation and deacylation events.

作者信息

Agudo-Ibáñez Lorena, Herrero Ana, Barbacid Mariano, Crespo Piero

机构信息

Instituto de Biomedicina y Biotecnología de Cantabria (IBBTEC), Consejo Superior de Investigaciones Científicas (CSIC), Universidad de Cantabria, Departamento de Biología Molecular, Facultad de Medicina Santander, Cantabria, Spain.

Molecular Oncology Program, Centro Nacional de Investigaciones Oncológicas (CNIO), Madrid, Spain.

出版信息

Mol Cell Biol. 2015 Jun 1;35(11):1898-914. doi: 10.1128/MCB.01398-14. Epub 2015 Mar 16.

Abstract

H-Ras must adhere to the plasma membrane to be functional. This is accomplished by posttranslational modifications, including palmitoylation, a reversible process whereby H-Ras traffics between the plasma membrane and the Golgi complex. At the plasma membrane, H-Ras has been proposed to occupy distinct sublocations, depending on its activation status: lipid rafts/detergent-resistant membrane fractions when bound to GDP, diffusing to disordered membrane/soluble fractions in response to GTP loading. Herein, we demonstrate that H-Ras sublocalization is dictated by its degree of palmitoylation in a cell type-specific manner. Whereas H-Ras localizes to detergent-resistant membrane fractions in cells with low palmitoylation activity, it locates to soluble membrane fractions in lineages where it is highly palmitoylated. Interestingly, in both cases GTP loading results in H-Ras diffusing away from its original sublocalization. Moreover, tilting the equilibrium between palmitoylation and depalmitoylation processes can substantially alter H-Ras segregation and, subsequently, its biochemical and biological functions. Thus, the palmitoylation/depalmitoylation balance not only regulates H-Ras cycling between endomembranes and the plasma membrane but also serves as a key orchestrator of H-Ras lateral diffusion between different types of plasma membrane and thereby of H-Ras signaling.

摘要

H-Ras必须附着于质膜才能发挥功能。这是通过翻译后修饰来实现的,包括棕榈酰化,这是一个可逆过程,通过该过程H-Ras在质膜和高尔基体复合体之间穿梭。在质膜上,根据其激活状态,H-Ras被认为占据不同的亚定位:与GDP结合时位于脂筏/抗去污剂膜组分中,响应GTP加载扩散到无序膜/可溶组分中。在此,我们证明H-Ras的亚定位以细胞类型特异性方式由其棕榈酰化程度决定。在棕榈酰化活性低的细胞中,H-Ras定位于抗去污剂膜组分,而在高度棕榈酰化的谱系中,它定位于可溶膜组分。有趣的是,在这两种情况下,GTP加载都会导致H-Ras从其原始亚定位扩散开来。此外,改变棕榈酰化和去棕榈酰化过程之间的平衡可显著改变H-Ras的分离,进而改变其生化和生物学功能。因此,棕榈酰化/去棕榈酰化平衡不仅调节H-Ras在内膜和质膜之间的循环,还作为H-Ras在不同类型质膜之间侧向扩散的关键协调者,从而调节H-Ras信号传导。

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