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Kinetic insulation as an effective mechanism for achieving pathway specificity in intracellular signaling networks

机译:动力学绝缘是在细胞内信号网络中实现途径特异性的有效机制

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摘要

Intracellular signaling pathways that share common components often elicit distinct physiological responses. In most cases, the biochemical mechanisms responsible for this signal specificity remain poorly understood. Protein scaffolds and cross-inhibition have been proposed as strategies to prevent unwanted cross-talk. Here, we report a mechanism for signal specificity termed “kinetic insulation.” In this approach signals are selectively transmitted through the appropriate pathway based on their temporal profile. In particular, we demonstrate how pathway architectures downstream of a common component can be designed to efficiently separate transient signals from signals that increase slowly over time. Furthermore, we demonstrate that upstream signaling proteins can generate the appropriate input to the common pathway component regardless of the temporal profile of the external stimulus. Our results suggest that multilevel signaling cascades may have evolved to modulate the temporal profile of pathway activity so that stimulus information can be efficiently encoded and transmitted while ensuring signal specificity.
机译:共有共同成分的细胞内信号传导途径常常引起不同的生理反应。在大多数情况下,导致这种信号特异性的生化机制仍然知之甚少。已经提出蛋白质支架和交叉抑制作为防止有害串扰的策略。在这里,我们报告了一种称为“运动隔离”的信号特异性机制。在这种方法中,基于信号的时间轮廓,通过适当的路径选择性地传输信号。特别是,我们演示了如何设计通用组件下游的通道架构,以有效地将瞬态信号与随时间缓慢增加的信号分开。此外,我们证明上游信号蛋白可以生成适当的输入到公共途径的组成部分,而不考虑外部刺激的时间概况。我们的研究结果表明,多级信号传导级联可能已经发展为调节途径活动的时间分布,从而可以在确保信号特异性的同时有效地编码和传输刺激信息。

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