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PDCD4 inhibits translation initiation by binding to eIF4A using both its MA3 domains

机译:PDCD4通过使用两个MA3结构域与eIF4A结合来抑制翻译启动

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摘要

Programmed Cell Death 4 (PDCD4) is a protein known to bind eukaryotic initiation factor 4A (eIF4A), inhibit translation initiation, and act as a tumor suppressor. PDCD4 contains two C-terminal MA3 domains, which are thought to be responsible for its inhibitory function. Here, we analyze the structures and inhibitory functions of these two PDCD4 MA3 domains by x-ray crystallography, NMR, and surface plasmon resonance. We show that both MA3 domains are structurally and functionally very similar and bind specifically to the eIF4A N-terminal domain (eIF4A-NTD) using similar binding interfaces. We found that the PDCD4 MA3 domains compete with the eIF4G MA3 domain and RNA for eIF4A binding. Our data provide evidence that PDCD4 inhibits translation initiation by displacing eIF4G and RNA from eIF4A. The PDCD4 MA3 domains act synergistically to form a tighter and more stable complex with eIF4A, which explains the need for two tandem MA3 domains.
机译:程序性细胞死亡4(PDCD4)是一种已知可结合真核起始因子4A(eIF4A),抑制翻译起始并充当肿瘤抑制因子的蛋白质。 PDCD4包含两个C末端MA3结构域,被认为是其抑制功能的原因。在这里,我们通过X射线晶体学,NMR和表面等离振子共振分析了这两个PDCD4 MA3域的结构和抑制功能。我们显示这两个MA3域在结构和功能上都非常相似,并使用相似的结合界面特异性结合到eIF4A N末端域(eIF4A-NTD)。我们发现,PDCD4 MA3域与eIF4G MA3域和RNA竞争eIF4A结合。我们的数据提供了PDCD4通过置换eIF4G和来自eIF4A的RNA抑制翻译起始的证据。 PDCD4 MA3结构域协同作用,与eIF4A形成更紧密,更稳定的复合体,这说明了需要两个串联的MA3结构域。

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