Picornaviral IRES elements are essential for initiating the cap-independent viral translation. However, three-dimensional structures of these elements remain elusive. Here, we report a 2.84-Ã resolution crystal structure of hepatitis A virus IRES domain V (dV) in complex with a synthetic antibody fragment-a crystallization chaperone. The RNA adopts a three-way junction structure, topologically organized by an adenine-rich stem-loop motif. Despite no obvious sequence homology, the dV architecture shows a striking similarity to a circularly permuted form of encephalomyocarditis virus J-K domain, suggesting a conserved strategy for organizing the domain architecture. Recurrence of the motif led us to use homology modeling tools to compute a 3-dimensional structure of the corresponding domain of foot-and-mouth disease virus, revealing an analogous domain organizing motif. The topological conservation observed among these IRESs and other viral domains implicates a structured three-way junction as an architectural scaffold to pre-organize helical domains for recruiting the translation initiation machinery.
A conserved RNA structural motif for organizing topology within picornaviral internal ribosome entry sites.
用于组织小核糖核酸病毒内部核糖体进入位点拓扑结构的保守RNA结构基序
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作者:Koirala Deepak, Shao Yaming, Koldobskaya Yelena, Fuller James R, Watkins Andrew M, Shelke Sandip A, Pilipenko Evgeny V, Das Rhiju, Rice Phoebe A, Piccirilli Joseph A
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2019 | 起止号: | 2019 Aug 9; 10(1):3629 |
| doi: | 10.1038/s41467-019-11585-z | 种属: | Viral |
| 研究方向: | 其它 | ||
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