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IκB-NF-κB信号转导模块:时间控制与选择性基因激活

The IkappaB-NF-kappaB signaling module: temporal control and selective gene activation.

作者信息

Hoffmann Alexander, Levchenko Andre, Scott Martin L, Baltimore David

机构信息

Division of Biology, California Institute of Technology, Pasadena, CA 91125, USA.

出版信息

Science. 2002 Nov 8;298(5596):1241-5. doi: 10.1126/science.1071914.

Abstract

Nuclear localization of the transcriptional activator NF-kappaB (nuclear factor kappaB) is controlled in mammalian cells by three isoforms of NF-kappaB inhibitor protein: IkappaBalpha, -beta, and - epsilon. Based on simplifying reductions of the IkappaB-NF-kappaB signaling module in knockout cell lines, we present a computational model that describes the temporal control of NF-kappaB activation by the coordinated degradation and synthesis of IkappaB proteins. The model demonstrates that IkappaBalpha is responsible for strong negative feedback that allows for a fast turn-off of the NF-kappaB response, whereas IkappaBbeta and - epsilon function to reduce the system's oscillatory potential and stabilize NF-kappaB responses during longer stimulations. Bimodal signal-processing characteristics with respect to stimulus duration are revealed by the model and are shown to generate specificity in gene expression.

摘要

转录激活因子核因子κB(NF-κB)的核定位在哺乳动物细胞中受NF-κB抑制蛋白的三种亚型调控:IκBα、IκBβ和IκBε。基于基因敲除细胞系中IκB-NF-κB信号模块的简化还原,我们提出了一个计算模型,该模型描述了通过IκB蛋白的协同降解和合成对NF-κB激活的时间控制。该模型表明,IκBα负责强大的负反馈,从而实现NF-κB反应的快速关闭,而IκBβ和IκBε的作用是降低系统的振荡潜能,并在较长时间刺激期间稳定NF-κB反应。该模型揭示了关于刺激持续时间的双峰信号处理特性,并显示其在基因表达中产生特异性。

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