The Leader RNA of Coronavirus Mouse Hepatitis Virus Contains an Enhancer-Like Element for Subgenomic mRNA Transcription

doi:10.1128/JVI.74.22.10571-10580.2000

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Journal of Virology, November 2000, p. 10571-10580, Vol. 74, No. 22
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

The Leader RNA of Coronavirus Mouse Hepatitis Virus Contains an Enhancer-Like Element for Subgenomic mRNA Transcription

Yicheng Wang and Xuming Zhang^*

Department of Microbiology and Immunology, University of Arkansas for Medical Sciences, Little Rock, Arkansas 72205

Received 28 April 2000/Accepted 15 August 2000

While the 5' cis-acting sequence of mouse hepatitis virus (MHV) for genomic RNA replication has been determined in severaldefective interfering (DI) RNA systems, it remains elusive forsubgenomic RNA transcription. Previous studies have shown thatthe leader RNA in the DI genome significantly enhances the efficiencyof DI subgenomic mRNA transcription, indicating that the leaderRNA is a cis-acting sequence for mRNA transcription. To furthercharacterize the cis-acting sequence, we made a series of deletionmutants, all but one of which have an additional deletion of thecis-acting signal for replication in the 5' untranslated region.This deletion effectively eliminated the replication of the DI-chloramphenicolacetyltransferase (CAT)-reporter, as demonstrated by the sensitivereverse transcription (RT)-PCR. The ability of these replication-minusmutants to transcribe subgenomic mRNAs was then assessed usingthe DI RNA-CAT reporter system. Results from both CAT activityand mRNA transcripts detected by RT-PCR showed that a 5'-proximalsequence of 35 nucleotides (nt) at nt 25 to 59 is a cis-actingsequence required for subgenomic RNA transcription, while theconsensus repeat sequence of the leader RNA does not have sucheffect. Analyses of the secondary structure indicate that this35-nt sequence forms two stem-loops conserved among MHVs. Deletionof this sequence abrogated transcriptional activity and disruptedthe predicted stem-loops and overall RNA secondary structure atthe 5' untranslated region, suggesting that the secondary structureformed by this 35-nt sequence may facilitate the downstream consensussequence accessible for the discontinuous RNA transcription. Thismay provide a mechanism by which the 5' cis-acting sequence regulatessubgenomic RNA transcription. The 5'-most 24 nt are not essentialfor transcription, while the 9 nt immediately downstream of theleader enhances RNA transcription. The sequence between nt 86and 135 had little effect on transcription. This study thus definesthe cis-acting transcription signal at the 5' end of the DIgenome.

^* Corresponding author. Mailing address: Department of Microbiology and Immunology, University of Arkansas for Medical Sciences,4301 W. Markham St., Slot 511, Little Rock, AR 72205. Phone: (501)686-7415. Fax: (501) 686-5359. E-mail: zhangxuming{at}exchange.uams.edu.

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