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RNA helicase DDX19 stabilizes ribosomal elongation and termination complexes

机译:RNA解旋酶DDX19稳定核糖体延伸和终止复合物

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摘要

The human DEAD-box RNA-helicase DDX19 functions in mRNA export through the nuclear pore complex. The yeast homolog of this protein, Dbp5, has been reported to participate in translation termination. Using a reconstituted mammalian in vitro translation system, we show that the human protein DDX19 is also important for translation termination. It is associated with the fraction of translating ribosomes. We show that DDX19 interacts with pre-termination complexes (preTCs) in a nucleotide-dependent manner. Furthermore, DDX19 increases the efficiency of termination complex (TC) formation and the peptide release in the presence of eukaryotic release factors. Using the eRF1(AGQ) mutant protein or a non-hydrolysable analog of GTP to inhibit subsequent peptidyl-tRNA hydrolysis, we reveal that the activation of translation termination by DDX19 occurs during the stop codon recognition. This activation is a result of DDX19 binding to preTC and a concomitant stabilization of terminating ribosomes. Moreover, we show that DDX19 stabilizes ribosome complexes with translation elongation factors eEF1 and eEF2. Taken together, our findings reveal that the human RNA helicase DDX19 actively participates in protein biosynthesis.
机译:人DEAD-box RNA解旋酶DDX19在通过核孔复合体输出的mRNA中起作用。据报道,该蛋白质的酵母同源物Dbp5参与翻译终止。使用重构的哺乳动物体外翻译系统,我们显示人蛋白质DDX19对翻译终止也很重要。它与翻译核糖体的比例有关。我们显示DDX19以核苷酸依赖性方式与预终止复合物(preTCs)相互作用。此外,DDX19在真核生物释放因子存在下提高了终止复合物(TC)形成和肽释放的效率。使用eRF1(AGQ)突变蛋白或GTP的不可水解类似物来抑制随后的肽基-tRNA水解,我们揭示了由DDX19激活的翻译终止在终止密码子识别过程中发生。该激活是DDX19与preTC结合以及末端核糖体随之稳定的结果。此外,我们显示DDX19稳定具有翻译延伸因子eEF1和eEF2的核糖体复合物。两者合计,我们的发现表明,人类RNA解旋酶DDX19积极参与蛋白质的生物合成。

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