蛋白质工程
变构调节
计算生物学
融合蛋白
多样性(控制论)
蛋白质设计
生物
计算机科学
蛋白质结构
遗传学
人工智能
生物化学
基因
重组DNA
受体
酶
作者
Amelia C. McCue,Brian Kuhlman
标识
DOI:10.1016/j.sbi.2022.102377
摘要
Engineered, light-sensitive protein switches are used to interrogate a broad variety of biological processes. These switches are typically constructed by genetically fusing naturally occurring light-responsive protein domains with functional domains from other proteins. Protein activity can be controlled using a variety of mechanisms including light-induced colocalization, caging, and allosteric regulation. Protein design efforts have focused on reducing background signaling, maximizing the change in activity upon light stimulation, and perturbing the kinetics of switching. It is common to combine structure-based modeling with experimental screening to identify ideal fusion points between domains and discover point mutations that optimize switching. Here, we introduce commonly used light-sensitive domains and summarize recent progress in using them to regulate protein activity.
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