Influenza A Virus Defective Viral Genomes Are Inefficiently Packaged into Virions Relative to Wild-Type Genomic RNAs
Autor: | William K. Reiser, Christopher B. Brooke, Aartjan J. W. te Velthuis, Fadi G. Alnaji, Joel Rivera-Cardona |
---|---|
Jazyk: | angličtina |
Rok vydání: | 2021 |
Předmět: |
RNA-dependent RNA polymerase
Genome Viral genome packaging Biology Virus Replication medicine.disease_cause Microbiology Virus 03 medical and health sciences chemistry.chemical_compound defective interfering particles Virology Influenza Human Extracellular Influenza A virus medicine Humans 030304 developmental biology 0303 health sciences 030306 microbiology Virion Wild type RNA Viral Genome Packaging sequencing Uridine QR1-502 3. Good health chemistry RNA Viral Defective Interfering Viruses influenza Intracellular Research Article |
Zdroj: | mBio, Vol 12, Iss 6 (2021) mBio |
ISSN: | 2150-7511 |
DOI: | 10.1128/mBio.02959-21 |
Popis: | Deletion-containing viral genomes (DelVGs) are commonly produced during influenza A virus infection and have been implicated in influencing clinical infection outcomes. Despite their ubiquity, the specific molecular mechanisms that govern DelVG formation and their packaging into defective interfering particles (DIPs) remain poorly understood. Here, we utilized next-generation sequencing to analyze DelVGs that form de novo early during infection, prior to packaging. Analysis of these early DelVGs revealed that deletion formation occurs in clearly defined hot spots and is significantly associated with both direct sequence repeats and enrichment of adenosine and uridine bases. By comparing intracellular DelVGs with those packaged into extracellular virions, we discovered that DelVGs face a significant bottleneck during genome packaging relative to wild-type genomic RNAs. Interestingly, packaged DelVGs exhibited signs of enrichment for larger DelVGs suggesting that size is an important determinant of packaging efficiency. Our data provide the first unbiased, high-resolution portrait of the diversity of DelVGs that are generated by the influenza A virus replication machinery and shed light on the mechanisms that underly DelVG formation and packaging. IMPORTANCE Defective interfering particles (DIPs) are commonly produced by RNA viruses and have been implicated in modulating clinical infection outcomes; hence, there is increasing interest in the potential of DIPs as antiviral therapeutics. For influenza viruses, DIPs are formed by the packaging of genomic RNAs harboring internal deletions. Despite decades of study, the mechanisms that drive the formation of these deletion-containing viral genomes (DelVGs) remain elusive. Here, we used a specialized sequencing pipeline to characterize the first wave of DelVGs that form during influenza virus infection. This data set provides an unbiased profile of the deletion-forming preferences of the influenza virus replicase. In addition, by comparing the early intracellular DelVGs to those that get packaged into extracellular virions, we described a significant segment-specific bottleneck that limits DelVG packaging relative to wild-type viral RNAs. Altogether, these findings reveal factors that govern the production of both DelVGs and DIPs during influenza virus infection. |
Databáze: | OpenAIRE |
Externí odkaz: |