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Dynamic modelling of the mTOR signalling network reveals complex emergent behaviours conferred by DEPTOR

机译:mTOR信号网络的动态建模揭示了DEPTOR赋予的复杂紧急行为

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The mechanistic Target of Rapamycin (mTOR) signalling network is an evolutionarily conserved network that controls key cellular processes, including cell growth and metabolism. Consisting of the major kinase complexes mTOR Complex 1 and 2 (mTORC1/2), the mTOR network harbours complex interactions and feedback loops. The DEP domain-containing mTOR-interacting protein (DEPTOR) was recently identified as an endogenous inhibitor of both mTORC1 and 2 through direct interactions, and is in turn degraded by mTORC1/2, adding an extra layer of complexity to the mTOR network. Yet, the dynamic properties of the DEPTOR-mTOR network and the roles of DEPTOR in coordinating mTORC1/2 activation dynamics have not been characterised. Using computational modelling, systems analysis and dynamic simulations we show that DEPTOR confers remarkably rich and complex dynamic behaviours to mTOR signalling, including abrupt, bistable switches, oscillations and co-existing bistable/oscillatory responses. Transitions between these distinct modes of behaviour are enabled by modulating DEPTOR expression alone. We characterise the governing conditions for the observed dynamics by elucidating the network in its vast multi-dimensional parameter space, and develop strategies to identify core network design motifs underlying these dynamics. Our findings provide new systems-level insights into the complexity of mTOR signalling contributed by DEPTOR.
机译:雷帕霉素(mTOR)信号传递机制的靶标是一种进化保守的网络,可控制关键的细胞过程,包括细胞生长和代谢。由主要的激酶复合物mTOR复合物1和2(mTORC1 / 2)组成,mTOR网络包含复杂的相互作用和反馈回路。含有DEP结构域的mTOR相互作用蛋白(DEPTOR)最近通过直接相互作用被鉴定为mTORC1和2的内源性抑制剂,进而被mTORC1 / 2降解,为mTOR网络增加了一层额外的复杂性。然而,尚未描述DEPTOR-mTOR网络的动态特性以及DEPTOR在协调mTORC1 / 2激活动力学中的作用。通过使用计算建模,系统分析和动态仿真,我们表明DEPTOR赋予mTOR信号显着丰富而复杂的动态行为,包括突然的双稳态开关,振荡和共存的双稳态/振荡响应。通过单独调制DEPTOR表达,可以在这些不同的行为模式之间进行转换。我们通过在庞大的多维参数空间中阐明网络来表征观察到的动力学的控制条件,并开发策略来识别这些动力学背后的核心网络设计主题。我们的发现为DEPTOR贡献的mTOR信号复杂性提供了新的系统级见解。

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