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Initiation factor 2 crystal structure reveals a different domain organization from eukaryotic initiation factor 5B and mechanism among translational GTPases

机译:起始因子2的晶体结构揭示了与真核起始因子5B不同的结构域和翻译GTPases之间的机制

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摘要

The initiation of protein synthesis uses initiation factor 2 (IF2) in prokaryotes and a related protein named eukaryotic initiation factor 5B (eIF5B) in eukaryotes. IF2 is a GTPase that positions the initiator tRNA on the 30S ribosomal initiation complex and stimulates its assembly to the 50S ribosomal subunit to make the 70S ribosome. The 3.1-Å resolution X-ray crystal structures of the full-length Thermus thermophilus apo IF2 and its complex with GDP presented here exhibit two different conformations (all of its domains except C2 domain are visible). Unlike all other translational GTPases, IF2 does not have an effecter domain that stably contacts the switch II region of the GTPase domain. The domain organization of IF2 is inconsistent with the “articulated lever” mechanism of communication between the GTPase and initiator tRNA binding domains that has been proposed for eIF5B. Previous cryo-electron microscopy reconstructions, NMR experiments, and this structure show that IF2 transitions from being flexible in solution to an extended conformation when interacting with ribosomal complexes.
机译:蛋白质合成的起始在原核生物中使用起始因子2(IF2),在真核生物中使用名为真核生物起始因子5B(eIF5B)的相关蛋白。 IF2是一种GTP酶,可将启动子tRNA定位在30S核糖体起始复合体上,并刺激其装配到50S核糖体亚基上,形成70S核糖体。此处显示的全长嗜热栖热菌apo IF2的3.1-A分辨率X射线晶体结构及其与GDP的复合物表现出两种不同的构象(除C2域外,其他所有域均可见)。与所有其他翻译GTPases不同,IF2没有稳定连接GTPase域的switch II区域的效应子域。 IF2的域组织与已针对eIF5B提出的GTPase和起始tRNA结合域之间的“铰接杠杆”通信机制不一致。先前的低温电子显微镜重建,NMR实验和这种结构表明,当与核糖体复合物相互作用时,IF2从溶液中的柔性过渡到扩展的构象。

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