RNA in-situ hybridization for pathology-based diagnosis of feline infectious peritonitis (FIP): current diagnostics for FIP and comparison to the current gold standard

Sweet, Arjun; André, Nicole M.; Whittaker, Gary; Licitra, Beth N.

doi:10.32388/nun8kb.2

“…Histological detection like immunohistochemistry (IHC) and in-situ hybridization target the N protein ( i . e ., antibody FIPV3-70) and RdRp (39), respectively. While targeting these genes can be useful for detection purposes ( i .…”

Section: Introductionmentioning

confidence: 99%

“…For example, commonly used serology tests target the N protein (31), and detection by RT-PCR targets genes like the RNA-dependent RNA polymerase (RdRp, (35) or 7a and 7b (38) (Figure 1). Histological detection like immunohistochemistry (IHC) and in-situ hybridization target the N protein (i.e., antibody FIPV3-70) and RdRp (39), respectively. While targeting these genes can be useful for detection purposes (i.e., they are highly conserved), they are not optimal for differentiating FCoV-1 and -2 (Figure 1).…”

Section: Introductionmentioning

confidence: 99%

“…For each tissue, an unstained slide of 5 m thick tissue sections were used. A probe directed to the RdRp gene(39) was used to detect FCoV RNA by in-situ hybridization (ISH, RNAscope ® Probe V-FIPV-ORF1a1b, Advanced Cell Diagnostics). The ISH process was carried out at the AHDC in the automated staining platform Ventana Discovery Ultra (Roche Tissue Diagnostics) using the Discovery kits for mRNA Sample Prep, mRNA Red Probe Amplification and mRNA Red Detection and the Ventana Hematoxylin and Ventana Bluing Reagents for counterstaining.Approximately 40 mg of each tissue was used for RNA extraction using the Monarch ® Total RNA Miniprep Kit (New England Biolabs, NEB) according to the manufacturer's instructions and including the suggested DNaseI…”

mentioning

confidence: 99%

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Molecular detection using hybridization capture and next-generation sequencing reveals cross-species transmission of feline coronavirus type-1 between a domestic cat and a captive wild felid

Olarte-Castillo,

Goodman,

Whittaker

2024

Preprint

0

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Feline coronavirus (FCoV) infection normally causes mild or subclinical signs and is common in domestic cats. However, in some cats, FCoV infection can also lead to the development of feline infectious peritonitis (FIP), a typically lethal disease. FCoV has two serotypes or genotypes, FCoV-1 and FCoV-2, both of which can cause FIP. The main difference between the genotypes is the viral spike (S) protein that determines tropism and pathogenicity, crucial mechanisms in the development of FIP. Subclinical infection and FIP have both been reported in wild felids, including in threatened species. Due to the high genetic variability of the S gene and the technical challenges to sequencing it, detection and characterization of FCoV in wild felids have mainly centered on other more conserved genes. Therefore, the genotype causing FIP in most wild felids remains unknown. Here, we report a retrospective molecular epidemiological investigation of FCoV in a zoological institution in the United States. In 2008, a domestic cat (Felis catus) and a Pallas cat (Otocolobus manul) sharing the same room succumbed to FIP. Using hybridization capture and next-generation sequencing, we detected and sequenced the complete 3-end of the viral genome (~8.2 Kb), including the S gene, from both felids. Our data show for the first time that FCoV-1 can be transmitted between domestic and wild felids and extends the known host range of FCoV-1. Our findings highlight the importance of identifying the genotype causing FIP, to develop effective control measures.

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“…To date, these viruses are still considered fatal for young cats, and therapies are mainly based on antiviral nucleotides like remdesivir and its analogs. However, no prophylaxis or vaccine is available [ 2 , 3 ]; in fact, cases of antibody-dependent enhancement (ADE) of FIPV infectivity have been observed following the development of the humoral response, which facilitates the entry of the virus in the macrophages, where the pathogen amplifies its replication [ 4 , 5 , 6 ].…”

Section: Introductionmentioning

confidence: 99%

An Exploratory Bioinformatic Investigation of Cats’ Susceptibility to Coronavirus-Deriving Epitopes

Buonocore,

De Biase,

Sorrentino

et al. 2024

Life

0

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Coronaviruses are highly transmissible and pathogenic viruses for humans and animals. The vast quantity of information collected about SARS-CoV-2 during the pandemic helped to unveil details of the mechanisms behind the infection, which are still largely elusive. Recent research demonstrated that different class I/II human leukocyte antigen (HLA) alleles might define an individual susceptibility to SARS-CoV-2 spreading, contributing to the differences in the distribution of the infection through different populations; additional studies suggested that the homolog of the HLA in cats, the feline leukocyte antigen (FLA), plays a pivotal role in the transmission of viruses. With these premises, this study aimed to exploit a bioinformatic approach for the prediction of the transmissibility potential of two distinct feline coronaviruses (FCoVs) in domestic cats (feline enteric coronavirus (FeCV) and feline infectious peritonitis virus (FIPV)) using SARS-CoV-2 as the reference model. We performed an epitope mapping of nonapeptides deriving from SARS-CoV-2, FeCV, and FIPV glycoproteins and predicted their affinities for different alleles included in the three main loci in class I FLAs (E, H, and K). The predicted complexes with the most promising affinities were then subjected to molecular docking and molecular dynamics simulations to provide insights into the stability and binding energies in the cleft. Results showed the FLA proteins encoded by alleles in the FLA-I H (H*00501 and H*00401) and E (E*01001 and E*00701) loci are largely responsive to several epitopes deriving from replicase and spike proteins of the analyzed coronaviruses. The analysis of the most affine epitope sequences resulting from the prediction can stimulate the development of anti-FCoV immunomodulatory strategies based on peptide drugs.

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Molecular detection using hybridization capture and next-generation sequencing reveals cross-species transmission of feline coronavirus type-1 between a domestic cat and a captive wild felid

Olarte-Castillo,

Goodman,

Whittaker

2024

Microbiol Spectr

0

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Feline coronavirus (FCoV) infection normally causes mild or subclinical signs and is common in domestic cats. However, in some cats, FCoV infection can also lead to the development of feline infectious peritonitis (FIP)—a typically lethal disease. FCoV has two serotypes or genotypes, FCoV-1 and FCoV-2, both of which can cause FIP. The main difference between the genotypes is the viral spike (S) protein that determines tropism and pathogenicity, crucial mechanisms in the development of FIP. Subclinical infection and FIP have both been reported in wild felids, including in threatened species. Due to the high genetic variability of the S gene and the technical challenges to sequencing it, detection and characterization of FCoV in wild felids have mainly centered on other more conserved genes. Therefore, the genotype causing FIP in most wild felids remains unknown. Here, we report a retrospective molecular epidemiological investigation of FCoV in a zoological institution in the U.Ss. In 2008, a domestic cat ( Felis catus ) and a Pallas’ cat ( Otocolobus manul ) sharing the same room succumbed to FIP. Using in situ hybridization, we detected FCoV RNA in different tissues of both felids. Using hybridization capture and next-generation sequencing, we detected, sequenced, and characterized the whole genome of the FCoV infecting both felids. Our data show for the first time that FCoV-1 can be transmitted between domestic and wild felids and extends the known host range of FCoV-1. Our findings highlight the importance of identifying the genotype causing FIP, to develop effective control measures. IMPORTANCE Feline coronavirus (FCoV) is highly prevalent in domestic cats worldwide and has also been reported in wild felids, including endangered species, in which it has caused substantial population declines. Characterizing the genetic diversity of FCoV is crucial due to recent reports of novel pathogenic recombinant variants causing high mortality in feral cats in Cyprus. In this retrospective molecular epidemiology study, we used archived samples collected in a zoological institution in the U.S. in which a domestic and a wild felid succumbed to FCoV. Using hybridization capture (HC) and next-generation sequencing, we show for the first time that FCoV can be naturally transmitted between domestic and wild felids. We demonstrate the efficacy of HC for detecting and sequencing the whole genome of FCoV, which is essential to characterize its different genotypes.

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RNA in-situ hybridization for pathology-based diagnosis of feline infectious peritonitis (FIP): current diagnostics for FIP and comparison to the current gold standard

Cited by 3 publications

References 32 publications

Molecular detection using hybridization capture and next-generation sequencing reveals cross-species transmission of feline coronavirus type-1 between a domestic cat and a captive wild felid

Molecular detection using hybridization capture and next-generation sequencing reveals cross-species transmission of feline coronavirus type-1 between a domestic cat and a captive wild felid

An Exploratory Bioinformatic Investigation of Cats’ Susceptibility to Coronavirus-Deriving Epitopes

Molecular detection using hybridization capture and next-generation sequencing reveals cross-species transmission of feline coronavirus type-1 between a domestic cat and a captive wild felid

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