Mutation of neutralizing/antibody-dependent enhancing epitope on spike protein and 7b gene of feline infectious peritonitis virus: Influences of viral replication in monocytes/macrophages and virulence in cats

Takano, Tomomi; Tomiyama, Yoshika; Katoh, Yasuichiroh; Nakamura, M.; Satoh, Ryoichi; Hohdatsu, Tsutomu

doi:10.1016/j.virusres.2010.12.020

Cited by 29 publications

(34 citation statements)

References 27 publications

(44 reference statements)

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“…The occurrence of FIP is thought to be largely affected by viral virulence factors, and their roles in FIP have been intensely studied. Several viral genes, including spike [31][32][33], accessory gene 3c [34][35][36] and 7b [37][38][39], and membrane [40], have been proposed to play important roles in the development of the disease in FCoV-infected cats. As a disease with immunopathogenesis entity, the knowledge of the host genetic factors that affect FIP is still very limited, and only two studies have reported such factors [41,42], in contrast to the considerable quantity of information on the virulence factors.…”

Section: Discussionmentioning

confidence: 99%

Identification and genotyping of feline infectious peritonitis-associated single nucleotide polymorphisms in the feline interferon-γ gene

Hsieh

Chueh

2014

Vet Res

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Feline infectious peritonitis (FIP) is an immune-mediated, highly lethal disease caused by feline coronavirus (FCoV) infection. Currently, no protective vaccine or effective treatment for the disease is available. Studies have found that some cats survive the challenge of virulent FCoV isolates. Since cellular immunity is thought to be critical in preventing FIP and because diseased cats often show a significant decrease in interferon-γ (IFN-γ) production, we investigated whether single nucleotide polymorphisms (SNP) in the feline IFN-γ gene (fIFNG) are associated with the outcome of infection. A total of 82 asymptomatic and 63 FIP cats were analyzed, and 16 SNP were identified in intron 1 of fIFNG. Among these SNP, the fFING + 428 T allele was shown to be a FIP-resistant allele (p = 0.03), and the heterozygous genotypes 01C/T and +408C/T were found to be FIP-susceptible factors (p = 0.004). Furthermore, an fIFNG + 428 resistant allele also showed a clear correlation with the plasma level of IFN-γ in FIP cats. For the identification of these three FIP-related SNP, genotyping methods were established using amplification refractory mutation system PCR (ARMS-PCR) and restriction fragment length polymorphisms (RFLP), and the different genotypes could easily be identified without sequencing. The identification of additional FIP-related SNP will allow the selection of resistant cats and decrease the morbidity of the cat population to FIP.

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Section: Discussionmentioning

confidence: 99%

Identification and genotyping of feline infectious peritonitis-associated single nucleotide polymorphisms in the feline interferon-γ gene

Hsieh

Chueh

2014

Vet Res

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“…Out of 30 peptides derived from this region that were tested in mice, four peptides that included both Th1 and Th2 epitopes were identified; the authors concluded that these regions should be explored in cats as potential immunogens. Takano et al (2011b) also studied the putative ADE epitopes in FIPV WSU-79-1146 with a battery of monoclonal antibodies against the virus neutralizing epitope on the S protein. Virus cultures exposed to one of these monoclonal antibodies eventually yielded a virus with two amino acid changes in the neutralizing epitope of the S protein that rendered it resistant to neutralization.…”

Section: Antibody-dependent Enhancementmentioning

confidence: 99%

An update on feline infectious peritonitis: Virology and immunopathogenesis

Pedersen

2014

The Veterinary Journal

174

264

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Feline infectious peritonitis (FIP) continues to be one of the most researched infectious diseases of cats. The relatively high mortality of FIP, especially for younger cats from catteries and shelters, should be reason enough to stimulate such intense interest. However, it is the complexity of the disease and the grudging manner in which it yields its secrets that most fascinate researchers. Feline leukemia virus infection was conquered in less than two decades and the mysteries of feline immunodeficiency virus were largely unraveled in several years. After a half century, FIP remains one of the last important infections of cats for which we have no single diagnostic test, no vaccine and no definitive explanations for how virus and host interact to cause disease. How can a ubiquitous and largely non-pathogenic enteric coronavirus transform into a highly lethal pathogen? What are the interactions between host and virus that determine both disease form (wet or dry) and outcome (death or resistance)? Why is it so difficult, and perhaps impossible, to develop a vaccine for FIP? What role do genetics play in disease susceptibility? This review will explore research conducted over the last 5 years that attempts to answer these and other questions. Although much has been learned about FIP in the last 5 years, the ultimate answers remain for yet more studies.

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“…93 RT-PCR cannot discriminate between FECV and FIPV due to the various single nucleotide polymorphisms (SNPs) and deletion mutations present in both biotypes, sometimes even identified from the same cat. 46,164,165 At the time of writing, no specific genetic determinants that trigger the evolution of FECV to FIPV or otherwise distinguish the 2 biotypes have been confirmed. Due to these particularities of FCoV, a specific RT-PCR for FIPV cannot, as yet, be designed.…”

Section: Rt-pcrmentioning

confidence: 99%

Feline Coronavirus in Multicat Environments

Drechsler

Alcaraz

Bossong

et al. 2011

Veterinary Clinics of North America: Small Animal Practice

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Feline infectious peritonitis (FIP), a fatal disease in cats worldwide, is caused by FCoV infection, which commonly occurs in multicat environments. The enteric FCoV, referred to as feline enteric virus (FECV), is considered a mostly benign biotype infecting the gut, whereas the FIP virus biotype is considered the highly pathogenic etiologic agent for FIP. Current laboratory tests are unable to distinguish between virus biotypes of FCoV. FECV is highly contagious and easily spreads in multicat environments; therefore, the challenges to animal shelters are tremendous. This review summarizes interdisciplinary current knowledge in regard to virology, immunology, pathology, diagnostics, and treatment options in the context of multicat environments.

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Mutation of neutralizing/antibody-dependent enhancing epitope on spike protein and 7b gene of feline infectious peritonitis virus: Influences of viral replication in monocytes/macrophages and virulence in cats

Cited by 29 publications

References 27 publications

Identification and genotyping of feline infectious peritonitis-associated single nucleotide polymorphisms in the feline interferon-γ gene

Identification and genotyping of feline infectious peritonitis-associated single nucleotide polymorphisms in the feline interferon-γ gene

An update on feline infectious peritonitis: Virology and immunopathogenesis

Feline Coronavirus in Multicat Environments

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