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Development of novel metabolite-responsive transcription factors via transposon-mediated protein fusion

机译:通过转座子介导的蛋白融合开发新型代谢物应答转录因子

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摘要

Naturally evolved metabolite-responsive biosensors enable applications in metabolic engineering, ranging from screening large genetic libraries to dynamically regulating biosynthetic pathways. However, there are many metabolites for which a natural biosensor does not exist. To address this need, we developed a general method for converting metabolite-binding proteins into metabolite-responsive transcription factors—Biosensor Engineering by Random Domain Insertion (BERDI). This approach takes advantage of an in vitro transposon insertion reaction to generate all possible insertions of a DNA-binding domain into a metabolite-binding protein, followed by fluorescence activated cell sorting to isolate functional biosensors. To develop and evaluate the BERDI method, we generated a library of candidate biosensors in which a zinc finger DNA-binding domain was inserted into maltose binding protein, which served as a model well-studied metabolite-binding protein. Library diversity was characterized by several methods, a selection scheme was deployed, and ultimately several distinct and functional maltose-responsive transcriptional biosensors were identified. We hypothesize that the BERDI method comprises a generalizable strategy that may ultimately be applied to convert a wide range of metabolite-binding proteins into novel biosensors for applications in metabolic engineering and synthetic biology.
机译:自然进化的代谢物响应型生物传感器可用于代谢工程,从筛选大型基因库到动态调节生物合成途径。但是,有许多代谢物不存在天然生物传感器。为了满足这一需求,我们开发了一种将代谢物结合蛋白转化为代谢物响应性转录因子的通用方法-通过随机域插入(BERDI)进行生物传感器工程设计。这种方法利用了体外转座子插入反应来将DNA结合域插入到代谢物结合蛋白中,然后进行荧光激活的细胞分选以分离功能性生物传感器。为了开发和评估BERDI方法,我们生成了候选生物传感器库,其中将锌指DNA结合结构域插入麦芽糖结合蛋白中,该蛋白作为模型研究的代谢物结合蛋白。文库的多样性通过几种方法进行了表征,采用了选择方案,最终鉴定出了几种独特的功能性麦芽糖反应性转录生物传感器。我们假设BERDI方法包括一种可推广的策略,该策略最终可用于将各种代谢物结合蛋白转化为用于代谢工程和合成生物学的新型生物传感器。

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