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RNA Mimicry by the Fap7 Adenylate Kinase in Ribosome Biogenesis

机译:Fap7腺苷酸激酶在核糖体生物发生中的RNA模拟。

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摘要

During biogenesis of the 40S and 60S ribosomal subunits, the pre-40S particles are exported to the cytoplasm prior to final cleavage of the 20S pre-rRNA to mature 18S rRNA. Amongst the factors involved in this maturation step, Fap7 is unusual, as it both interacts with ribosomal protein Rps14 and harbors adenylate kinase activity, a function not usually associated with ribonucleoprotein assembly. Human hFap7 also regulates Cajal body assembly and cell cycle progression via the p53–MDM2 pathway. This work presents the functional and structural characterization of the Fap7–Rps14 complex. We report that Fap7 association blocks the RNA binding surface of Rps14 and, conversely, Rps14 binding inhibits adenylate kinase activity of Fap7. In addition, the affinity of Fap7 for Rps14 is higher with bound ADP, whereas ATP hydrolysis dissociates the complex. These results suggest that Fap7 chaperones Rps14 assembly into pre-40S particles via RNA mimicry in an ATP-dependent manner. Incorporation of Rps14 by Fap7 leads to a structural rearrangement of the platform domain necessary for the pre-rRNA to acquire a cleavage competent conformation.
机译:在40S和60S核糖体亚基的生物合成过程中,在将20S pre-rRNA最终切割为成熟的18S rRNA之前,将pre-40S颗粒输出到细胞质。在此成熟步骤涉及的因素中,Fap7是不寻常的,因为它既与核糖体蛋白Rps14相互作用,又具有腺苷酸激酶活性,该功能通常与核糖核蛋白装配无关。人类hFap7还通过p53–MDM2途径调节Cajal体组装和细胞周期进程。这项工作介绍了Fap7–Rps14复合物的功能和结构表征。我们报告说,Fap7协会阻止Rps14的RNA结合表面,相反,Rps14结合抑制Fap7的腺苷酸激酶活性。此外,Fap7对Rps14的亲和力与结合的ADP较高,而ATP水解则使复合物解离。这些结果表明,Fap7分子伴侣Rps14通过RNA模仿以ATP依赖的方式组装成40S以前的颗粒。 Fap7掺入Rps14导致pre-rRNA获得裂解感受态构象所需的平台结构域的结构重排。

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