Article ; Online: The aberrant gene-end transcription signal of the matrix M gene of human parainfluenza virus type 3 downregulates fusion F protein expression and the F-specific antibody response in vivo.
2015 Volume 89, Issue 6, Page(s) 3318–3331
Abstract: ... transcript of the M gene and the downstream fusion (F) protein gene. We hypothesized that this insert ... may function to downregulate the expression of F protein by interfering with termination/reinitiation at the M ... F gene junction, thus promoting the production of M-F readthrough mRNA at the expense ...
Abstract | Unlabelled: Human parainfluenza virus type 3 (HPIV3), a paramyxovirus, is a major viral cause of severe lower respiratory tract disease in infants and children. The gene-end (GE) transcription signal of the HPIV3 matrix (M) protein gene is identical to those of the nucleoprotein and phosphoprotein genes except that it contains an apparent 8-nucleotide insert. This was associated with an increased synthesis of a readthrough transcript of the M gene and the downstream fusion (F) protein gene. We hypothesized that this insert may function to downregulate the expression of F protein by interfering with termination/reinitiation at the M-F gene junction, thus promoting the production of M-F readthrough mRNA at the expense of monocistronic F mRNA. To test this hypothesis, two similar recombinant HPIV3 viruses from which this insert in the M-GE signal was removed were generated. The M-GE mutants exhibited a reduction in M-F readthrough mRNA and an increase in monocistronic F mRNA. This resulted in a substantial increase in F protein synthesis in infected cells as well as enhanced incorporation of F protein into virions. The efficiency of mutant virus replication was similar to that of wild-type (wt) HPIV3 both in vitro and in vivo. However, the F-protein-specific serum antibody response in hamsters was increased for the mutants compared to wt HPIV3. This study identifies a previously undescribed viral mechanism for attenuating the host adaptive immune response. Repairing the M-GE signal should provide a means to increase the antibody response to a live attenuated HPIV3 vaccine without affecting viral replication and attenuation. Importance: The HPIV3 M-GE signal was previously shown to contain an apparent 8-nucleotide insert that was associated with increased synthesis of a readthrough mRNA of the M gene and the downstream F gene. However, whether this had any significant effect on the synthesis of monocistronic F mRNA or F protein, virus replication, virion morphogenesis, and immunogenicity was unknown. Here, we show that the removal of this insert shifts F gene transcription from readthrough M-F mRNA to monocistronic F mRNA. This resulted in a substantial increase in the amount of F protein expressed in the cell and packaged in the virus particle. This did not affect virus replication but increased the F-specific antibody response in hamsters. Thus, in wild-type HPIV3, the aberrant M-GE signal operates a previously undescribed mechanism that reduces the expression of a major neutralization and protective antigen, resulting in reduced immunogenicity. This has implications for the design of live attenuated HPIV3 vaccines; specifically, the antibody response against F can be elevated by "repairing" the M-GE signal to achieve higher-level F antigen expression, with no effect on attenuation. |
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MeSH term(s) | Animals ; Antibodies, Viral/immunology ; Base Sequence ; Cricetinae ; Down-Regulation ; Gene Expression Regulation, Viral ; Humans ; Mesocricetus ; Molecular Sequence Data ; Parainfluenza Virus 3, Human/genetics ; Parainfluenza Virus 3, Human/immunology ; Respirovirus Infections/immunology ; Respirovirus Infections/virology ; Transcription, Genetic ; Viral Fusion Proteins/genetics ; Viral Fusion Proteins/immunology ; Viral Matrix Proteins/genetics ; Viral Matrix Proteins/immunology |
Chemical Substances | Antibodies, Viral ; Viral Fusion Proteins ; Viral Matrix Proteins |
Language | English |
Publishing date | 2015-03 |
Publishing country | United States |
Document type | Journal Article ; Research Support, N.I.H., Intramural |
ZDB-ID | 80174-4 |
ISSN | 1098-5514 ; 0022-538X |
ISSN (online) | 1098-5514 |
ISSN | 0022-538X |
DOI | 10.1128/JVI.03148-14 |
Database | MEDical Literature Analysis and Retrieval System OnLINE |
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