期刊论文详细信息
PeerJ
Independent evolution of tetraloop in enterovirus oriL replicative element and its putative binding partners in virus protein 3C
article
Maria A. Prostova1  Andrei A. Deviatkin1  Irina O. Tcelykh1  Alexander N. Lukashev1  Anatoly P. Gmyl1 
[1] Chumakov Institute of Poliomyelitis and Viral Encephalitides;Lomonosov Moscow State University;Sechenov First Moscow State Medical University
关键词: Enterovirus;    RNA-protein interaction;    Tetraloop;    Virus evolution;   
DOI  :  10.7717/peerj.3896
学科分类:社会科学、人文和艺术(综合)
来源: Inra
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【 摘 要 】

BackgroundEnteroviruses are small non-enveloped viruses with a (+) ssRNA genome with one open reading frame. Enterovirus protein 3C (or 3CD for some species) binds the replicative element oriL to initiate replication. The replication of enteroviruses features a low-fidelity process, which allows the virus to adapt to the changing environment on the one hand, and requires additional mechanisms to maintain the genome stability on the other. Structural disturbances in the apical region of oriL domain d can be compensated by amino acid substitutions in positions 154 or 156 of 3C (amino acid numeration corresponds to poliovirus 3C), thus suggesting the co-evolution of these interacting sequences in nature. The aim of this work was to understand co-evolution patterns of two interacting replication machinery elements in enteroviruses, the apical region of oriL domain d and its putative binding partners in the 3C protein.Methods6, 400 nucleotides), which were present in the NCBI database on February 2017 and analysed the variety and abundance of sequences in domain d of the replicative element oriL and in the protein 3C.ResultsA total of 2,842 full genome sequences was analysed. The majority of domain d apical loops were tetraloops, which belonged to consensus YNHG (Y = U/C, N = any nucleotide, H = A/C/U). The putative RNA-binding tripeptide 154–156 (Enterovirus C 3C protein numeration) was less diverse than the apical domain d loop region and, in contrast to it, was species-specific.DiscussionDespite the suggestion that the RNA-binding tripeptide interacts with the apical region of domain d, they evolve independently in nature. Together, our data indicate the plastic evolution of both interplayers of 3C-oriL recognition.

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