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KH domains with impaired nucleic acid binding as a tool for functional analysis

机译:核酸结合受损的KH结构域可作为功能分析的工具

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In eukaryotes, RNA-binding proteins that contain multiple K homology (KH) domains play a key role in coordinating the different steps of RNA synthesis, metabolism and localization. Understanding how the different KH modules participate in the recognition of the RNA targets is necessary to dissect the way these proteins operate. We have designed a KH mutant with impaired RNA-binding capability for general use in exploring the role of individual KH domains in the combinatorial functional recognition ofRNA targets. A double mutation in the hallmark GxxG loop (GxxG-to-GDDG) impairs nucleic acid binding without compromising the stability of the domain. We analysed the impact of the GDDG mutations in individual KH domains on the functional properties ofKSRP as a prototype of multiple KH domain-containing proteins. We show how the GDDG mutant can be used to directly link biophysical information on the sequence specificity of the different KH domains of KSRP and their role in mRNA recognition and decay.This work defines a general molecular biology tool for the investigation of the function of individual KH domains in nucleic acid binding proteins.
机译:在真核生物中,包含多个K同源性(KH)域的RNA结合蛋白在协调RNA合成,代谢和定位的不同步骤中起着关键作用。了解不同的KH模块如何参与RNA靶标的识别对于剖析这些蛋白的运作方式是必要的。我们设计了一种具有受损的RNA结合能力的KH突变体,可用于探索单个KH域在RNA靶标的组合功能识别中的作用。标志性的GxxG环中的双重突变(GxxG到GDDG)会损害核酸结合而不损害域的稳定性。我们分析了单个KH域中GDDG突变对KSRP的功能特性的影响,KSRP作为多个包含KH域的蛋白质的原型。我们展示了如何使用GDDG突变体直接链接有关KSRP不同KH域的序列特异性及​​其在mRNA识别和衰变中的作用的生物物理信息。这项工作定义了用于研究个体功能的通用分子生物学工具核酸结合蛋白中的KH结构域。

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