Reproductive disorders in boars infected experi-mentally with porcine parvovirus
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Abstract:
ミニチュア雄豚5ヵ月齢3頭を用い,実験的にPPVに感染させた雄豚について造精機能に及ぼす影響を病理組織学的に検討した。雄豚はPPVの感染によって明瞭な臨床症状を現さなかった。また,生殖器には病理組織学的に著変がなかったが,精巣における軽度の造精障害,精巣上体,精嚢腺,精索などにおける軽度の炎症性変化が注目された。従って,本症の感染が造精機能を低下させる他の要因と重複した場合には,異常精液の生産を招来することが示唆された。Keywords:
Porcine parvovirus
Summary The antigenic relatedness of minute virus of mice (MVM), Kilham rat virus (KR), H-1 virus (H-1), haemorrhagic encephalopathy of rats virus (HER), porcine parvovirus (PPV), canine parvovirus (CPV), feline panleukopenia virus (FPV), goose parvovirus (GPV) and bovine parvovirus (BPV) was studied by immunofluorescence microscopy (FA) and by serum neutralization (SN). An antigenically related group comprising MVM, KR, HER, PPV, CPV and FPV was recognized by FA and most reactions within the group were reciprocal. Antigenic relatedness was less evident when the same viruses and antisera were tested by SN. Only CPV and FPV were closely and reciprocally related. Other cross-reactions by SN were quantitatively minor and included neutralization of CPV and FPV by pig anti-PPV serum and neutralization of H-1 and HER by rat anti-KR serum. Neither FA nor SN revealed any antigenic relationship of BPV and GPV either with each other or with any of the other viruses tested.
Canine parvovirus
Porcine parvovirus
Immunofluorescence
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Human parvovirus 4 (PARV4), a recently discovered parvovirus found exclusively in human plasma and liver tissue, was considered phylogenetically distinct from other parvoviruses. Here, we report the discovery of two novel parvoviruses closely related to PARV4, porcine hokovirus (PHoV) and bovine hokovirus (BHoV), from porcine and bovine samples in Hong Kong. Their nearly full-length sequences were also analysed. PARV4-like viruses were detected by PCR among 44.4 % (148/333) of porcine samples (including lymph nodes, liver, serum, nasopharyngeal and faecal samples), 13 % (4/32) of bovine spleen samples and 2 % (7/362) of human serum samples that were sent for human immunodeficiency virus and hepatitis C virus antibody tests. Three distinct parvoviruses were identified, including two novel parvoviruses, PHoV and BHoV, from porcine and bovine samples and PARV4 from humans, respectively. Analysis of genome sequences from seven PHoV strains, from three BHoV strains and from one PARV4 strain showed that the two animal parvoviruses were most similar to PARV4 with 61.5-63 % nt identities and, together with PARV4 (HHoV), formed a distinct cluster within the family Parvoviridae. The three parvoviruses also differed from other parvoviruses by their relatively large predicted VP1 protein and the presence of a small unique conserved putative protein. Based on these results, we propose a separate genus, Hokovirus, to describe these three parvoviruses. The co-detection of porcine reproductive and respiratory syndrome virus, the agent associated with the recent 'high fever' disease outbreaks in pigs in China, from our porcine samples warrants further investigation.
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Porcine parvovirus
Canine parvovirus
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A recombinant baculovirus containing the NS1 gene of minute virus of mice was constructed. Optimal expression of the recombinant NS1 protein (rNS1) was achieved by infecting Trichoplusa ni High Five cells at a multiplicity of 10 and incubating them for 72 h postinfection. An enzyme-linked immunosorbent assay (ELISA) with rNS1 as the antigen was evaluated for serologic testing of laboratory rodents. The rNS1 ELISA proved to be a more sensitive method for the detection of antibodies to recently recognized rodent parvovirus species (mouse orphan parvovirus and rat orphan parvovirus) and prototypic parvovirus species (minute virus of mice, Kilham's rat virus, and H-1) than were conventional parvovirus ELISAs that use whole parvovirus virions.
Porcine parvovirus
Recombinant virus
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Porcine parvovirus
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The construction and characterization of a full-length infectious plasmid clone of the newly identified hamster parvovirus (HaPV) are described. Following transfection of hamster BHK cells with the infectious clone, pHaPV, the specific intracellular DNA replicative forms, RNA transcripts and viral proteins that were expected for this rodent parvovirus were generated. Infected cells were lysed and progeny virus was produced, demonstrating that pHaPV could generate a productive virus infection. The complete sequences of both hairpin termini, which had not been previously determined, were obtained. Preliminary host-range studies, which compared virus production and macromolecular synthesis in various cell lines following either HaPV infection or pHaPV transfection, demonstrated an early block of infection of HaPV in both monkey COS-1 and murine A9 cells. The availability of an HaPV infectious clone will facilitate its genetic analysis and allow the elucidation of the determinants important in host range, tissue tropism and pathogenicity of this newly identified rodent parvovirus.
clone (Java method)
Porcine parvovirus
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To obtain a bivalence vaccine against canine rabies virus and canine parvovirus, a chimeric rabies virus expressing canine parvovirus VP2 protein was generated by the technique of reverse genetics. It was shown that the chimeric virus designated as HEP-Flury (VP2) grew well on BHK-21 cells and the VP2 gene could still be stably expressed after ten passages on BHK-21 cells. Experiments on the mice immunized with the chimeric virus HEP-Flury (VP2) demonstrated that specific antibodies against rabies virus and canine parvovirus were induced in immunized mice after vaccination with the live chimeric virus.
Canine parvovirus
Porcine parvovirus
Duck embryo vaccine
Lyssavirus
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Inactivated feline parvovirus vaccine produced in a continuous feline cell line evoked a protective canine parvovirus antibody titer and prevented virus shedding following challenge in previously seronegative puppies. Post-vaccinal reactions to the vaccine were not observed in laboratory puppies vaccinated with multiple doses of vaccine or in vaccinated puppies from 5 clinics and/or animal shelters.
Canine parvovirus
Inactivated vaccine
Porcine parvovirus
Viral Shedding
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Inactivated whole-virus vaccines against porcine parvovirus (PPV) can prevent disease but not infection and virus shedding after heterologous virus challenge. Here, we showed that the same is true for a homologous challenge. Pregnant sows were vaccinated with an experimental inactivated vaccine based on PPV strain 27a. They were challenged on day 40 of gestation with the virulent porcine parvovirus PPV-27a from which the vaccine was prepared (homologous challenge). On day 90 of gestation, the fetuses from vaccinated sows were protected against disease, while the fetuses of the non-vaccinated sows (control group) exhibited signs of parvovirus disease. All gilts, whether vaccinated or not vaccinated, showed a boost of PPV-specific antibodies indicative of virus infection and replication. Low DNA copy numbers, but not infectious virus, could be demonstrated in nasal or rectal swabs of immunized sows, but high copy numbers of challenge virus DNA as well as infectious virus could both be demonstrated in non-vaccinated sows.
Porcine parvovirus
Viral Shedding
Heterologous
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Canine parvovirus
Recombinant virus
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