Abstract

Pokeweed antiviral protein (PAP) is a ribosome-inactivating protein isolated from the pokeweed plant (Phytolacca americana) that inhibits the proliferation of several plant and animal viruses. We have shown previously that PAP and nontoxic mutants of PAP can directly depurinate brome mosaic virus (BMV) RNA in vitro, resulting in reduced viral protein translation. Here we expand on these initial studies and, using a barley protoplast system, demonstrate that recombinant PAP and nontoxic mutants isolated from E. coli are able to reduce the accumulation of BMV RNAs in vivo. Pretreatment of only BMV RNA3 with PAP prior to transfection of barley protoplasts reduced the accumulation of all BMV RNAs, with a more severe effect on subgenomic RNA4 levels. Using in vitro RNA synthesis assays, we show that a depurinated template causes the BMV replicase to stall at the template nucleotide adjacent to the missing base. These results provide new insight into the antiviral mechanism of PAP, namely that PAP depurination of BMV RNA impedes both RNA replication and subgenomic RNA transcription. These novel activities are distinct from the PAP-induced reduction of viral RNA translation and represent new targets for the inhibition of viral infection.

Highlights

  • Pokeweed antiviral protein (PAP)1 is a 29-kDa ribosomeinactivating protein of the pokeweed plant Phytolacca americana

  • Synthesis of Mature PAP and PAP Mutants in E. coli—In pokeweed, PAP is first synthesized as a 313-amino acid-long precursor that is processed to produce the mature (262-amino acid) form of the protein, which has 22 and 29 amino acids cleaved from the N and C termini, respectively

  • These results indicate that prior incubation of brome mosaic virus (BMV) RNAs with PAP inhibits the accumulation of these RNAs in barley protoplasts

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Summary

Introduction

Pokeweed antiviral protein (PAP)1 is a 29-kDa ribosomeinactivating protein of the pokeweed plant Phytolacca americana. PAP and nontoxic mutants reduced the accumulation of BMV RNAs in protoplasts, by inhibiting both viral RNA replication and transcription.

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