Affiliation:
1. Department of Biochemistry and Biophysics, Texas A&M University, College Station, Texas
Abstract
ABSTRACT
The
3′ portions of plus-strand brome mosaic virus (BMV) RNAs mimic
cellular tRNAs. Nucleotide substitutions or deletions in the 3′
CCA of the tRNA-like sequence (TLS) affect minus-strand initiation
unless repaired. We observed that 2-nucleotide deletions involving the
CCA 3′ sequence in one or all BMV RNAs still allowed RNA
accumulation in barley protoplasts at significant levels. Alterations
of CCA to GGA in only BMV RNA3 also allowed RNA accumulation at
wild-type levels. However, substitutions in all three BMV RNAs severely
reduced RNA accumulation, demonstrating that substitutions have
different repair requirements than do small deletions. Furthermore,
wild-type BMV RNA1 was required for the repair and replication of RNAs
with nucleotide substitutions. Results from sequencing of progeny viral
RNA from mutant input RNAs demonstrated that RNA1 did not contribute
its sequence to the mutant RNAs. Instead, the repaired ends were
heterogeneous, with one-third having a restored CCA and others having
sequences with the only commonality being the restoration of one
cytidylate. The role of BMV RNA1 in increased repair was
examined.
Publisher
American Society for Microbiology
Subject
Virology,Insect Science,Immunology,Microbiology
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