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Oncogenic re-wiring of cellular signaling pathways

机译:细胞信号通路的致癌性重布线

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Signaling pathways in mammalian cells are assembled and regulated by a finely controlled network of protein–protein and protein–phospholipid interactions, mediated by dedicated signaling domains and their cognate binding motifs. The domain-based modular architecture of signaling proteins may have facilitated the evolution of complex biological systems, and can be exploited experimentally to generate synthetic signaling pathways and artificial mechanisms of autoregulation. Pathogenic proteins, such as those encoded by bacteria and viruses, frequently form ectopic signaling complexes to respecify cellular behavior. In a similar fashion, proteins expressed as a consequence of oncogenic fusions, mutations or amplifications can elicit ectopic protein–protein interactions that re-wire signaling pathways, in a fashion that promotes malignancy. Compounds that directly or indirectly reverse these aberrant interactions offer new possibilities for therapy in cancer.
机译:哺乳动物细胞中的信号传导途径是由精细控制的蛋白质-蛋白质和蛋白质-磷脂相互作用网络组装和调节的,该网络由专用的信号传导域及其同源结合基序介导。信号蛋白的基于域的模块化体系结构可能已经促进了复杂生物系统的进化,并且可以通过实验加以利用以产生合成的信号通路和自动调节的人工机制。病原性蛋白质(例如由细菌和病毒编码的蛋白质)经常形成异位信号复合物,以重新指定细胞行为。以类似的方式,由于致癌融合,突变或扩增而表达的蛋白质可以引起异位蛋白质-蛋白质相互作用,从而以促进恶性的方式重新连接信号传导途径。直接或间接逆转这些异常相互作用的化合物为癌症治疗提供了新的可能性。

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