Aichi Virus Leader Protein Is Involved in Viral RNA Replication and Encapsidation

Sasaki, Jun; Nagashima, Shigeo; Taniguchi, Koki

doi:10.1128/jvi.77.20.10799-10807.2003

Cited by 36 publications

(26 citation statements)

References 44 publications

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“…The newly synthesized progeny RNA is encapsidated into the capsid proteins as soon as RNA is syn- thesized. In the case of Aichi virus, which belongs to the genus Kobuvirus of the family Picornaviridae, L is involved in viral RNA replication and encapsidation, since the accumulation of empty capsids was observed in the case of an L-deleted mutant virus (31). In this study, the peaks of empty capsids are almost similar among all the viruses.…”

Section: Discussionsupporting

confidence: 53%

Theiler's Murine Encephalomyelitis Virus Leader Protein Amino Acid Residue 57 Regulates Subgroup-Specific Virus Growth on BHK-21 Cells

Takano-Maruyama

Ohara

Asakura

et al. 2006

J Virol

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Strains of Theiler's murine encephalomyelitis virus (TMEV) are divided into two subgroups, TO and GDVII. TMEV strains show subgroup-specific virus growth and cell tropism and induce subgroup-specific diseases. Using site-directed mutagenesis, we demonstrated that the amino acid at position 57 of the leader protein (L 57 ), which is located at the most N-terminal part of the polyprotein, regulates subgroup-specific virus growth on BHK-21 cells. Further study suggested that L 57 may regulate viral RNA encapsidation, although it does not affect the synthesis of viral proteins or the assembly of viral intermediates.Theiler's murine encephalomyelitis virus (TMEV) belongs to the genus Cardiovirus of the family Picornaviridae and is divided into two subgroups on the basis of their different biological activities (23,26,30). GDVII subgroup strains cause acute and fatal polioencephalomyelitis in mice following intracerebral inoculation. In the few surviving mice, no virus persistence or demyelination is observed. In contrast, TO or DA subgroup strains induce a biphasic central nervous system disease. In the acute phase, the virus infects mainly neurons and causes mild polioencephalomyelitis. During the chronic phase, the virus persists in the spinal cord of susceptible strains of mice and causes demyelination. In addition, virus growth differs in vitro between strains of the two subgroups. On baby hamster kidney (BHK-21) cells, GDVII subgroup strains grow well at a titer that is 10-fold higher than that of DA subgroup strains. Furthermore, GDVII subgroup strains produce larger plaques (2.5 mm in diameter), whereas DA subgroup strains produce smaller plaques (less than 0.5 mm) (18).Leader protein (L) is located at the most N-terminal portion of the polyprotein in members of the Aphthovirus and Cardiovirus genera of the picornaviruses (17). L is known to enable virus growth on specific cell lines because it inhibits alpha/beta interferon (IFN-␣/␤) transcription (35). Although the capsid proteins have over 94% homology at the amino acid level, the homology of L between TO and GDVII subgroup strains is only 85% (20). The sequence difference between leader proteins of the two subgroups may account for TMEV subgroupspecific biological activities.There are 11 amino acid (aa) residue differences distributed over the total 76 aa of L between the two subgroup strains (20). One of the amino acid residues is proline, which is known to have an important influence on protein structure; cis-trans isomerization at a proline residue alters the protein structure. In addition, proline has the highest reverse turn probability (9). GDVII L contains eight proline residues, whereas DA L contains seven, since aa position 57 (L 57 ) is a proline in the case of the GDVII strain but is a serine in the case of the DA strain.We questioned whether the difference in L 57 regulates the structure of L and thereby affects TMEV subgroup-specific biological activities. Therefore, by generating a series of mutant viruses, we studied the possibility that L...

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Section: Discussionsupporting

confidence: 53%

Theiler's Murine Encephalomyelitis Virus Leader Protein Amino Acid Residue 57 Regulates Subgroup-Specific Virus Growth on BHK-21 Cells

Takano-Maruyama

Ohara

Asakura

et al. 2006

J Virol

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“…In fact, numerous attempts to identify an RNA encapsidation signal have failed. A single study reports that the encapsidation signal could lie within the 5′UTR of the Aichi virus together with the L protein 71 , 72 . However, a recent paper, which tends to favor the second model of encapsidation, also proposes a mechanism by which the triple interaction vRNA-2C-VP3 would be sufficient to explain the specificity of picornavirus encapsidation 73 .…”

Section: Viral Cyclementioning

confidence: 99%

The encephalomyocarditis virus

2012

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The encephalomyocarditis virus (EMCV) is a small non-enveloped single-strand RNA virus, the causative agent of not only myocarditis and encephalitis, but also neurological diseases, reproductive disorders and diabetes in many mammalian species. EMCV pathogenesis appears to be viral strain- and host-specific, and a better understanding of EMCV virulence factors is increasingly required. Indeed, EMCV is often used as a model for diabetes and viral myocarditis, and is also widely used in immunology as a double-stranded RNA stimulus in the study of Toll-like as well as cytosolic receptors. However, EMCV virulence and properties have often been neglected. Moreover, EMCV is able to infect humans albeit with a low morbidity. Progress on xenografts, such as pig heart transplantation in humans, has raised safety concerns that need to be explored. In this review we will highlight the biology of EMCV and all known and potential virulence factors.

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“…Aichi virus L and 2A functions remain unknown 3. L protein has no autocatalytic activity and is not involved in polyprotein cleavage, but is probably involved in both viral RNA replication and encapsidation 11. It was also reported that the 2A proteins of kobuviruses, as well as human parechoviruses and avian encephalomyelitis virus, have conserved motifs (H‐box/NC and transmembrane domain) that are characteristic of a family of cellular proteins (H‐rev107) involved in the control of cell proliferation 12 and in viral RNA replication 13.…”

Section: Genetic Structure and Function Of Kobuvirusesmentioning

confidence: 99%

Kobuviruses – a comprehensive review

Reuter

Boros

Pankovics

2011

Reviews in Medical Virology

165

144

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Kobuviruses are members of the large and growing family Picornaviridae. Until now, two official, Aichi virus and Bovine kobuvirus, and one candidate kobuvirus species, 'porcine kobuvirus', have been identified in human, cattle and swine, respectively. In addition, kobu-like viruses were detected very recently in the bat. Aichi virus could be one of the causative agents of gastroenteritis in humans, and kobuviruses probably also cause diarrhoea in cattle and swine. Although Aichi virus has been detected relatively infrequently (0-3%) in human diarrhoea, high seroprevalence, up to 80-95% at the age of 30-40, was found indicating the general nature of infection in different human populations. In the previous years, much new information has accumulated relating to kobuviruses and their host species. This review summarises the current knowledge on kobuviruses including taxonomy, biology and viral characteristics, and covers all aspects of infection including epidemiology, clinical picture, host species diversity, laboratory diagnosis and it gives a summary about possible future perspectives.

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Aichi Virus Leader Protein Is Involved in Viral RNA Replication and Encapsidation

Cited by 36 publications

References 44 publications

Theiler's Murine Encephalomyelitis Virus Leader Protein Amino Acid Residue 57 Regulates Subgroup-Specific Virus Growth on BHK-21 Cells

Theiler's Murine Encephalomyelitis Virus Leader Protein Amino Acid Residue 57 Regulates Subgroup-Specific Virus Growth on BHK-21 Cells

The encephalomyocarditis virus

Kobuviruses – a comprehensive review

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