| Literature DB >> 36069552 |
Isshu Kojima1,2, Koji Onomoto3, Wenjie Zuo4,5, Makoto Ozawa1,6,7, Kosuke Okuya1,7, Kiyotada Naitou8, Fumiki Izumi9,10, Misuzu Okajima9,10, Takuro Fujiwara10, Naoto Ito9,10, Mitsutoshi Yoneyama3,11, Kentaro Yamada12,13, Akira Nishizono14,15, Makoto Sugiyama10, Takashi Fujita4,5, Tatsunori Masatani9,10.
Abstract
Stress granules (SGs) are dynamic structures that store cytosolic messenger ribonucleoproteins. SGs have recently been shown to serve as a platform for activating antiviral innate immunity; however, several pathogenic viruses suppress SG formation to evade innate immunity. In this study, we investigated the relationship between rabies virus (RABV) virulence and SG formation, using viral strains with different levels of virulence. We found that the virulent Nishigahara strain did not induce SG formation, but its avirulent offshoot, the Ni-CE strain, strongly induced SG formation. Furthermore, we demonstrated that the amino acid at position 95 in the RABV matrix protein (M95), a pathogenic determinant for the Nishigahara strain, plays a key role in inhibiting SG formation, followed by protein kinase R (PKR)-dependent phosphorylation of the α subunit of eukaryotic initiation factor 2α (eIF2α). M95 was also implicated in the accumulation of RIG-I, a viral RNA sensor protein, in SGs and in the subsequent acceleration of interferon induction. Taken together, our findings strongly suggest that M95-related inhibition of SG formation contributes to the pathogenesis of RABV by allowing the virus to evade the innate immune responses of the host. IMPORTANCE Rabies virus (RABV) is a neglected zoonotic pathogen that causes lethal infections in almost all mammalian hosts, including humans. Recently, RABV has been reported to induce intracellular formation of stress granules (SGs), also known as platforms that activate innate immune responses. However, the relationship between SG formation capacity and pathogenicity of RABV has remained unclear. In this study, by comparing two RABV strains with completely different levels of virulence, we found that the amino acid mutation from valine to alanine at position 95 of matrix protein (M95), which is known to be one of the amino acid mutations that determine the difference in virulence between the strains, plays a major role in SG formation. Importantly, M95 was involved in the accumulation of RIG-I in SGs and in promoting interferon induction. These findings are the first report of the effect of a single amino acid substitution associated with SGs on viral virulence.Entities:
Keywords: interferons; rabies; stress granules
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Year: 2022 PMID: 36069552 PMCID: PMC9517722 DOI: 10.1128/jvi.00810-22
Source DB: PubMed Journal: J Virol ISSN: 0022-538X Impact factor: 6.549