Classical Swine Fever Virus Can Remain Virulent after Specific Elimination of the Interferon Regulatory Factor 3-Degrading Function of N
            <sup>pro</sup>

Ruggli, Nicolas; Summerfield, Artur; Fiebach, Ana R.; Guzylack‐Piriou, Laurence; Bauhofer, Oliver; Lamm, Catherine G.; Waltersperger, S.; Matsuno, Keita; Liu, Luzia; Gerber, Marlène; Choi, Kyung Hyun; Hofmann, Martin; Sakoda, Yoshihiro; Tratschin, Jon Duri

doi:10.1128/jvi.01509-08

Cited by 68 publications

(112 citation statements)

References 51 publications

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“…Whether restoring the N pro function in the triple mutant GPE Ϫ virus would further enhance its pathogenicity is under current investigation. Previous data suggest that the IRF3-degrading function of N pro may support the pathogenicity of low-and moderately virulent strains but has only little influence on the pathogenicity of highly virulent viruses: mutations to knock out the N pro -mediated IRF3 degradation did not alter the pathogenicity of the highly virulent CSFV strain Eystrup and resulted in only slight attenuation of the moderately virulent vA187-1 virus (43). E rns forms disulfide-linked homodimers and possesses RNase activity (45,50).…”

Section: Figmentioning

confidence: 99%

“…Comparison of the genomes of the GPE Ϫ vaccine virus and the parent ALD virus revealed 225 nucleotide substitutions and 46 amino acid differences (22), which did not provide any conclusive information on the molecular basis of the attenuation. Numerous reports suggest that the viral proteins N pro , C, E rns , E1, E2, p7, and NS4B may be involved in determining the virulence of CSFV in pigs (7,8,9,10,11,12,13,32,36,37,38,39,40,43,46,54). So far, however, all conclusions on CSFV virulence determinants rely on mutations that result in downregulation of pathogenicity.…”

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confidence: 99%

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Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

Tamura

Sakoda

Yoshino

et al. 2012

J Virol

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c Classical swine fever virus (CSFV) is the causative agent of classical swine fever (CSF), a highly contagious disease of pigs. There are numerous CSFV strains that differ in virulence, resulting in clinical disease with different degrees of severity. Low-virulent and moderately virulent isolates cause a mild and often chronic disease, while highly virulent isolates cause an acute and mostly lethal hemorrhagic fever. The live attenuated vaccine strain GPE ؊ was produced by multiple passages of the virulent ALD strain in cells of swine, bovine, and guinea pig origin. With the aim of identifying the determinants responsible for the attenuation, the GPE ؊ vaccine virus was readapted to pigs by serial passages of infected tonsil homogenates until prolonged viremia and typical signs of CSF were observed. The GPE ؊ /P-11 virus isolated from the tonsils after the 11th passage in vivo had acquired 3 amino acid substitutions in E2 (T830A) and NS4B (V2475A and A2563V) compared with the virus before passages. Experimental infection of pigs with the mutants reconstructed by reverse genetics confirmed that these amino acid substitutions were responsible for the acquisition of pathogenicity. Studies in vitro indicated that the substitution in E2 influenced virus spreading and that the changes in NS4B enhanced the viral RNA replication. In conclusion, the present study identified residues in E2 and NS4B of CSFV that can act synergistically to influence virus replication efficiency in vitro and pathogenicity in pigs.

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confidence: 99%

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confidence: 99%

Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

Tamura

Sakoda

Yoshino

et al. 2012

J Virol

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“…N pro (A187-1)/D136N showed higher stability than N pro (KPP)/S17P; N61K, although it was described to be defective in mediating IRF-3 degradation . This suggests that the lack of IRF-3 degradation by this TRASH domain mutant is indeed due to the lack of interaction with IRF-3 as described by Ruggli et al (2009) rather than to N pro instability, although a contribution by the latter cannot be excluded.…”

Section: Discussionmentioning

confidence: 77%

“…The KPP/93 strain showed low pathogenicity in pigs. In previous studies, the suppression of IFN-a/b induction by N pro was related to pathogenicity in pigs (Mayer et al, 2004;Ruggli et al, 2009;Tamura et al, 2014), suggesting that inability of KPP/93 N pro to suppress IFN-a/b induction may contribute to the low pathogenicity of the KPP/93 strain in pigs. In the present study, we identified amino acid residues of N pro responsible for the suppression of IFN-a/b induction by N pro .…”

Section: Discussionmentioning

confidence: 99%

“…The amino acid residues H49 and C69 in the N-terminal domain of N pro form a catalytic diad responsible for the autoprotease activity (Gottipati et al, 2013;Zögg et al, 2013). N pro is not essential for viral replication (Tratschin et al, 1998), but is involved in pathogenicity by suppressing IFN-a/b induction through IRF-3 degradation in host cells (Mayer et al, 2004;Hilton et al, 2006;Bauhofer et al, 2007;Ruggli et al, 2009;Tamura et al, 2014). A TRASH zinc-binding domain located in the C-terminal half of N pro , and involving the amino acid residues at positions 112, 134, 136 and 138, is required for mediating IRF-3 degradation Szymanski et al, 2009;Tamura et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

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The N-terminal domain of Npro of classical swine fever virus determines its stability and regulates type I IFN production

Mine

Tamura

Mitsuhashi³

et al. 2015

Journal of General Virology

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New Generation Self-Replicating RNA Vaccines Derived from Pestivirus Genome

Démoulins,

Techakriengkrai,

Ebensen

et al. 2024

RNA Vaccines

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Classical Swine Fever Virus Can Remain Virulent after Specific Elimination of the Interferon Regulatory Factor 3-Degrading Function of N ^pro

Cited by 68 publications

References 51 publications

Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

The N-terminal domain of Npro of classical swine fever virus determines its stability and regulates type I IFN production

New Generation Self-Replicating RNA Vaccines Derived from Pestivirus Genome

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Classical Swine Fever Virus Can Remain Virulent after Specific Elimination of the Interferon Regulatory Factor 3-Degrading Function of N pro

Cited by 68 publications

References 51 publications

Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

Selection of Classical Swine Fever Virus with Enhanced Pathogenicity Reveals Synergistic Virulence Determinants in E2 and NS4B

The N-terminal domain of Npro of classical swine fever virus determines its stability and regulates type I IFN production

New Generation Self-Replicating RNA Vaccines Derived from Pestivirus Genome

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Classical Swine Fever Virus Can Remain Virulent after Specific Elimination of the Interferon Regulatory Factor 3-Degrading Function of N ^pro