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Estrogen Receptor-α: Plasma Membrane Localization and Functions

机译:雌激素受体-α:血浆膜定位和功能

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The knowledge of the molecular mechanism by which estrogens exert pleiotropic functions in different tissues and organs has evolved rapidly during the past two decades. It is now well established that 17β-estradiol (E2) induces the transcriptional regulation of target gene expression upon binding to the intracellular estrogen receptor-α (ERα) or -β (ERb). In addition E2 modulates cell functions through rapid non-genomic actions. Stimulation of G-proteins, Ca2+ influx as well as phospholipase C, ERK/MAPK, and PI3K/AKT activation occur within seconds to minutes upon E2 binding to a small population of ERα located at the plasma membrane. Several laboratories have recently examined the structural requirements for the localization and function(s) of plasma membrane ERα. We have shown that human ERα location at the plasma membrane and its interaction with caveolin-1 is mediated by S-palmitoylation of the Cys447 residue. Moreover, E2 also modulates Cys447 S-(de)palmitoylation enabling ERα association with signal transduction proteins (e.g. Src and G-proteins) in a cell context-related fashion. This leads to downstream signaling important for cell growth and survival. Here, the structural bases and mechanisms for ERα localization and action(s) are discussed along with potential implications for development of new drugs.
机译:在过去的二十年中,关于雌激素在不同组织和器官中发挥多效功能的分子机理的知识发展迅速。现在已经确定17β-雌二醇(E2)在与细胞内雌激素受体-α(ERα)或-β(ERb)结合后诱导靶基因表达的转录调控。另外,E2通过快速的非基因组作用调节细胞功能。 E2与位于质膜上的一小部分ERα结合后,在几秒至几分钟内就会刺激G蛋白,Ca2 +内流以及磷脂酶C,ERK / MAPK和PI3K / AKT活化。最近有几个实验室检查了质膜ERα的定位和功能的结构要求。我们已经表明,人类ERα在质膜上的位置及其与小窝蛋白1的相互作用是由Cys447残基的S-棕榈酰化介导的。此外,E2还以细胞环境相关的方式调节Cys447 S-(去)棕榈糖基化,使ERα与信号转导蛋白(例如Src和G蛋白)结合。这导致对于细胞生长和存活重要的下游信号传导。在此,讨论了ERα定位和作用的结构基础和机制,以及对新药开发的潜在影响。

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