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RNA Remodeling Activity of DEAD Box Proteins Tuned by Protein Concentration, RNA Length, and ATP

机译:DEAD盒蛋白的RNA重塑活性通过蛋白浓度,RNA长度和ATP调节

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DEAD box RNA helicases play central roles in RNP biogenesis. We reported earlier that LAF-1, a DEAD box RNA helicase in C. elegans, dynamically interacts with RNA and that the interaction likely contributes to the fluidity of RNP droplets. Here we investigate the molecular basis of the interaction of RNA with LAF-1 and its human homolog, DDX3X. We show that both LAF-1 and DDX3X, at low concentrations, are monomers that induce tight compaction of single-stranded RNA. At high concentrations, the proteins are multimeric and dynamically interact with RNA in an RNA length-dependent manner. The dynamic LAF-1-RNA interaction stimulates RNA annealing activity. ATP adversely affects the RNA remodeling ability of LAF-1 by suppressing the affinity, dynamics, and annealing activity of LAF-1, suggesting that ATP may promote disassembly of the RNP complex. Based on our results, we postulate a plausible molecular mechanism underlying the dynamic equilibrium of the LAF-1 RNP complex.
机译:DEAD盒RNA解旋酶在RNP生物发生中起核心作用。我们之前报道过,LAF-1是秀丽隐杆线虫中的DEAD盒RNA解旋酶,它与RNA动态相互作用,这种相互作用可能有助于RNP小滴的流动性。在这里,我们研究了RNA与LAF-1及其人类同源物DDX3X相互作用的分子基础。我们显示低浓度的LAF-1和DDX3X都是诱导单链RNA紧密压缩的单体。在高浓度下,蛋白质是多聚体,并以RNA长度依赖性方式与RNA动态相互作用。动态LAF-1-RNA相互作用可刺激RNA退火活性。 ATP通过抑制LAF-1的亲和力,动力学和退火活性,对LAF-1的RNA重塑能力产生不利影响,这表明ATP可能会促进RNP复合物的分解。根据我们的结果,我们推测LAF-1 RNP复合物动态平衡的合理分子机制。

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