The Ser-2429-->Pro mutation in the nsp10 subunit of the EAV replicase severely impairs subgenomic positive- and negative-strand mRNA synthesis without affecting proteolytic processing.
The nsp10 subunit of the EAV replicase plays a critical role in an early step of viral subgenomic mRNA transcription.
Equine arteritis virus (EAV) is a positive-stranded RNA virus that synthesizes a 5'- and 3'-coterminal nested set of six subgenomic mRNAs. These mRNAs all contain a common leader sequence which is derived from the 5' end of the genome. Subgenomic mRNA transcription and genome replication are directed by the viral replicase, which is expressed in the form of two polyproteins and subsequently processed into smaller nonstructural proteins (nsps). During the recent construction of an EAV infectious cDNA clone (pEAV030 L. C. van Dinten, J. A. den Boon, A. L. M. Wassenaar, W. J. M. Spaan, and E. J. Snijder, Proc. Natl. Acad. Sci. USA 94:991-996, 1997), a mutant cDNA clone (pEAV030F) which carries a single replicase point mutation was obtained. This substitution (Ser-2429-->Pro) is located in the nsp10 subunit and renders the EAV030F virus deficient in subgenomic mRNA synthesis. To obtain more insight into the role of nsp10 in transcription and the nature of the transcriptional defect, we have now analyzed the EAV030F mutant in considerable detail. The Ser-2429-->Pro mutation does not affect the proteolytic processing of the replicase but apparently affects the function of nsp10 in transcription. Furthermore, our study showed that EAV030F still produces subgenomic positive and negative strands, albeit at a very low level. Both subgenomic positive-strand synthesis and negative-strand synthesis are equally affected by the Ser-2429-->Pro mutation, suggesting that nsp10 plays an important role in an early step of EAV mRNA transcription.
Marle et al. (Thu,) conducted a other in Equine arteritis virus (EAV) replication. Ser-2429-->Pro mutation in the nsp10 subunit vs. Wild-type EAV was evaluated on Subgenomic mRNA synthesis and proteolytic processing. The Ser-2429-->Pro mutation in the nsp10 subunit of the EAV replicase severely impairs subgenomic positive- and negative-strand mRNA synthesis without affecting proteolytic processing.
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