Human metapneumovirus M2-2 protein inhibits viral transcription and replication |
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| Authors: | Yoshinori Kitagawa Min Zhou Mayu Yamaguchi Takayuki Komatsu Kenji Takeuchi Masae Itoh Bin Gotoh |
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| Affiliation: | 1. Centre for Research and Knowledge Transfer in Biotechnology, University of Zagreb, Zagreb, Croatia;2. Center of Excellence for Viral Immunology and Vaccines, CERVirVac, Croatia;3. Dr. Andrija ?tampar Teaching Institute of Public Health, Zagreb, Croatia;4. University of Zagreb School of Medicine, Zagreb, Croatia;5. Croatian National Institute of Public Health, Zagreb, Croatia;1. Department of Microbiology and Immunology, Aichi Medical University School of Medicine, Nagakute, Aichi 480-1195, Japan;2. Department of Anatomy, Mongolian National University of Medical Sciences, Ulaanbaatar 210648, Mongolia |
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| Abstract: | M2-2 protein of human metapneumovirus (HMPV) is encoded by one of two overlapping open reading frames within M2 mRNA. The precise function of HMPV M2-2 protein remains unknown. We here examined effect of M2-2 protein on HMPV transcription and replication using a minigenome construct and monitoring luciferase reporter gene expression. The minigenome assays demonstrated that M2-2 protein inhibited both transcription and RNA replication. The inhibitory function of M2-2 protein was completely abrogated by removal of eight or four amino acids from its N- or C-terminus, respectively, demonstrating importance of both short terminal sequences for maintaining its functional structure. Immunoprecipitation experiments revealed interaction of M2-2 protein with L protein, which might be involved in inhibition of HMPV transcription and replication. Prior accumulation of intracellular M2-2 protein severely restrained HMPV from replicating. Thus inherent viral control of the M2-2 gene expression in infected cells seems to be essential for efficient HMPV replication. |
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