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The kinase activity of human Rio1 is required for final steps of cytoplasmic maturation of 40S subunits

机译:40S亚基细胞质成熟的最终步骤需要人Rio1的激酶活性

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RIO proteins form a conserved family of atypical protein kinases. Humans possess three distinct RIO kinases—hRio1, hRio2, and hRio3, of which only hRio2 has been characterized with respect to its role in ribosomal biogenesis. Here we show that both hRio1 and hRio3, like hRio2, are associated with precursors of 40S ribosomal subunits in human cells. Furthermore, we demonstrate that depletion of hRio1 by RNA interference affects the last step of 18S rRNA maturation and causes defects in the recycling of several trans -acting factors (hEnp1, hRio2, hLtv1, hDim2/PNO1, and hNob1) from pre-40S subunits in the cytoplasm. Although the effects of hRio1 and hRio2 depletion are similar, we show that the two kinases are not fully interchangeable. Moreover, rescue experiments with a kinase-dead mutant of hRio1 revealed that the kinase activity of hRio1 is essential for the recycling of the endonuclease hNob1 and its binding partner hDim2 from cytoplasmic pre-40S. Kinase-dead hRio1 is trapped on pre-40S particles containing hDim2 and hNob1 but devoid of hEnp1, hLtv1, and hRio2. These data reveal a role of hRio1 in the final stages of cytoplasmic pre-40S maturation.
机译:RIO蛋白形成一个保守的非典型蛋白激酶家族。人类拥有三种不同的RIO激酶-hRio1,hRio2和hRio3,其中只有hRio2在核糖体生物发生中的作用得到了表征。在这里,我们显示hRio1和hRio3与hRio2一样,都与人类细胞中40S核糖体亚基的前体有关。此外,我们证明了RNA干扰对hRio1的消耗会影响18S rRNA成熟的最后一步,并导致从40S之前的亚基回收几个反式作用因子(hEnp1,hRio2,hLtv1,hDim2 / PNO1和hNob1)的回收中存在缺陷。在细胞质中。尽管hRio1和hRio2耗竭的作用相似,但我们显示这两种激酶不是完全可互换的。此外,使用hRio1的激酶死亡突变体进行的抢救实验表明,hRio1的激酶活性对于核酸内切酶hNob1及其结合伴侣hDim2从细胞质40S的回收至关重要。死于激酶的hRio1被捕获在包含hDim2和hNob1但不含hEnp1,hLtv1和hRio2的40S前颗粒上。这些数据揭示了hRio1在细胞质40S提前成熟的最终阶段中的作用。

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