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Evolution of Synthetic Signaling Scaffolds by Recombination of Modular Protein Domains

机译:通过重组蛋白结构域的合成信号支架的演变。

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Signaling scaffolds are proteins that interact via modular domains with multiple partners, regulating signaling networks in space and time and providing an ideal platform from which to alter signaling functions. However, to better exploit scaffolds for signaling engineering, it is necessary to understand the full extent of their modularity. We used a directed evolution approach to identify, from a large library of randomly shuffled protein interaction domains, variants capable of rescuing the signaling defect of a yeast strain in which Ste5, the scaffold in the mating pathway, had been deleted. After a single round of selection, we identified multiple synthetic scaffold variants with diverse domain architectures, able to mediate mating pathway activation in a pheromone-dependent manner. The facility with which this signaling network accommodates changes in scaffold architecture suggests that the mating signaling complex does not possess a single, precisely defined geometry into which the scaffold has to fit. These relaxed geometric constraints may facilitate the evolution of signaling networks, as well as their engineering for applications in synthetic biology.
机译:信号支架是通过模块化结构域与多个配偶体相互作用的蛋白质,可在时空上调节信号网络,并为改变信号功能提供理想的平台。但是,为了更好地利用支架进行信号工程,必须了解其模块化的全部范围。我们使用了定向进化方法,从随机改组的蛋白质相互作用域的大型文库中,鉴定出能够挽救酵母菌株(其中交配途径中的支架Ste5已被删除)的信号缺陷的变体。经过一轮选择,我们确定了具有不同域结构的多个合成支架变体,能够以信息素依赖性方式介导交配途径的激活。该信号网络适应脚手架架构变化的设施表明,配对信号复合体不具备脚手架必须适合的单一,精确定义的几何形状。这些宽松的几何约束可以促进信号网络的发展以及它们在合成生物学中的应用工程。

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