首页> 美国卫生研究院文献>PLoS Biology >The DEAD-box Protein Rok1 Orchestrates 40S and 60S Ribosome Assembly by Promoting the Release of Rrp5 from Pre-40S Ribosomes to Allow for 60S Maturation
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The DEAD-box Protein Rok1 Orchestrates 40S and 60S Ribosome Assembly by Promoting the Release of Rrp5 from Pre-40S Ribosomes to Allow for 60S Maturation

机译:DEAD盒蛋白Rok1通过促进从40S以前的核糖体释放Rrp5到60S成熟来协调40S和60S核糖体装配。

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摘要

DEAD-box proteins are ubiquitous regulators of RNA biology. While commonly dubbed “helicases,” their activities also include duplex annealing, adenosine triphosphate (ATP)-dependent RNA binding, and RNA-protein complex remodeling. Rok1, an essential DEAD-box protein, and its cofactor Rrp5 are required for ribosome assembly. Here, we use in vivo and in vitro biochemical analyses to demonstrate that ATP-bound Rok1, but not adenosine diphosphate (ADP)-bound Rok1, stabilizes Rrp5 binding to 40S ribosomes. Interconversion between these two forms by ATP hydrolysis is required for release of Rrp5 from pre-40S ribosomes in vivo, thereby allowing Rrp5 to carry out its role in 60S subunit assembly. Furthermore, our data also strongly suggest that the previously described accumulation of snR30 upon Rok1 inactivation arises because Rrp5 release is blocked and implicate a previously undescribed interaction between Rrp5 and the DEAD-box protein Has1 in mediating snR30 accumulation when Rrp5 release from pre-40S subunits is blocked.
机译:DEAD-box蛋白是RNA生物学普遍存在的调节剂。尽管通常被称为“螺旋酶”,但它们的活性还包括双链退火,三磷酸腺苷(ATP)依赖性RNA结合以及RNA-蛋白质复合物重塑。 Rok1是必需的DEAD-box蛋白,其辅因子Rrp5是核糖体组装所必需的。在这里,我们使用体内和体外的生化分析来证明ATP结合的Rok1,而不是腺苷二磷酸(ADP)结合的Rok1,可以稳定Rrp5与40S核糖体的结合。在体内从40S前核糖体释放Rrp5时,需要通过ATP水解在这两种形式之间进行相互转化,从而使Rrp5发挥其在60S亚基装配中的作用。此外,我们的数据还强烈表明,Rok1失活后出现了先前描述的snR30积累,因为Rrp5释放受到阻滞,并且暗示了Rrp5和DEAD-box蛋白Has1之间先前未描述的相互作用,当Rrp5从40S之前的亚基释放时介导snR30积累。被阻止。

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