Fimmu-09-01581-g003

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Description: English: Transcription of the complimentary RNA (cRNA) and viral RNA (vRNA) by the heterotrimeric viral RNA-dependent RNA polymerase (PB2, PB1, and PA). (A) The viral polymerase initiates transcription of the positive-sense cRNA upon base-pairing of ATP and GTP with the complimentary nucleotides in the 3′ end of the vRNA. The subsequent formation of the A-G dinucleotide is followed by elongation of the cRNA transcript. Nucleoprotein (NP) molecules successively bind to the cRNA as it exits the polymerase, promoting cRNP assembly. cRNP formation is completed upon the termination of transcription and with the binding of a newly synthesized viral polymerase (yellow outline). (B) vRNA transcription proceeds in a similar manner as cRNA synthesis. Recent structures support a model where (i) ATP and GTP base pair to the nucleotides located 4 and 5 bases from the cRNA 3′ end, and there form a dinucleotide, which then disassociates and reanneals with the bases at positions 1 and 2. (ii) Alternatively, ATP and GTP could bind directly to the terminal nucleotides and form a dinucleotide. Both mechanisms would position the dinucleotide at the cRNA 3′ end, which is necessary to transcribe a full-length vRNA. Similar to cRNP formation, multiple NPs and a viral polymerase bind to the newly transcribed vRNA to produce a new viral ribonucleoprotein (vRNP). Date: 20 July 2018. Source: https://www.frontiersin.org/articles/10.3389/fimmu.2018.01581/full. Author: imageDan Dou, Rebecca Revol, Henrik Östbye, Hao Wang, and Robert Daniels.
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- imageDan Dou, Rebecca Revol, Henrik Östbye, Hao Wang, and Robert Daniels
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- imageDan Dou, Rebecca Revol, Henrik Östbye, Hao Wang, and Robert Daniels
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- https://www.frontiersin.org/articles/10.3389/fimmu.2018.01581/full
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