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The experimental power of FR900359 to study Gq-regulated biological processes

机译:FR900359研究Gq调控的生物过程的实验能力

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摘要

Despite the discovery of heterotrimeric alpha beta gamma G proteins similar to 25 years ago, their selective perturbation by cell-permeable inhibitors remains a fundamental challenge. Here we report that the plant-derived depsipeptide FR900359 (FR) is ideally suited to this task. Using a multifaceted approach we systematically characterize FR as a selective inhibitor of Gq/11/14 over all other mammalian G alpha isoforms and elaborate its molecular mechanism of action. We also use FR to investigate whether inhibition of Gq proteins is an effective post-receptor strategy to target oncogenic signalling, using melanoma as a model system. FR suppresses many of the hallmark features that are central to the malignancy of melanoma cells, thereby providing new opportunities for therapeutic intervention. Just as pertussis toxin is used extensively to probe and inhibit the signalling of Gi/o proteins, we anticipate that FR will at least be its equivalent for investigating the biological relevance of Gq.
机译:尽管发现了与25年前相似的异三聚体αβγG蛋白,但它们对细胞可渗透抑制剂的选择性摄动仍然是一项基本挑战。在这里我们报告说,植物衍生的二肽肽FR900359(FR)非常适合此任务。使用多方面的方法,我们系统地将FR表征为对所有其他哺乳动物Gα亚型的Gq / 11/14的选择性抑制剂,并阐述了其分子作用机理。我们还使用FR调查黑色素瘤作为模型系统,抑制Gq蛋白是否是靶向致癌信号的有效受体后策略。 FR抑制了许多黑色素瘤细胞恶性肿瘤的标志性特征,从而为治疗性干预提供了新的机会。正如百日咳毒素广泛用于探测和抑制Gi / o蛋白的信号传导一样,我们预计FR至少与研究Gq的生物学相关性相当。

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