Your search keyword '"Ohsawa, Kazutaka"' showing total 3 results

1. A single viral gene determines lethal cross-species neurovirulence of baboon herpesvirus HVP2.

Author

Black, Darla, Ohsawa, Kazutaka, Tyler, Shaun, Maxwell, Lara, and Eberle, R.

Subjects

*VIRAL genes, *MICROBIAL virulence, *HERPESVIRUSES, *LABORATORY mice, *NUCLEOTIDE sequence, *GENETIC recombination

Abstract

Abstract: Alpha-herpesviruses can produce more severe infections in non-natural host species than in their natural host. Isolates of the baboon alpha-herpesvirus Papiine herpesvirus 2 (HVP2) are either very neurovirulent in mice (subtype nv) or non-virulent (subtype ap), but no such difference is evident in the natural baboon host. Comparative genome sequencing was used to identify subtype-specific sequence differences (SSDs) between HVP2nv and HVP2ap isolates. Some genes were identified that despite exhibiting sequence variation among isolates did not have any SSDs, while other genes had comparatively high levels of SSDs. Construction of genomic recombinants between HVP2nv and HVP2ap isolates mapped the mouse neurovirulence determinant to within three genes. Construction of gene-specific recombinants demonstrated that the UL39 ORF is responsible for determining the lethal neurovirulence phenotype of HVP2 in mice. These results demonstrate that differences in a single viral gene can determine the severity of herpesvirus infection in a non-natural host species. [Copyright &y& Elsevier]

Published

2014

2. Genome sequence of a pathogenic isolate of monkey B virus (species Macacine herpesvirus 1).

Author

Ohsawa, Kazutaka, Black, Darla, Ohsawa, Makiko, and Eberle, R.

Subjects

*RHESUS monkeys, *HERPESVIRUS diseases in animals, *NUCLEOTIDE sequence, *VIRAL vaccines, *HERPES simplex virus, *VIRAL proteins, *DISEASES

Abstract

The only genome sequence for monkey B virus (BV; species Macacine herpesvirus 1) is that of an attenuated vaccine strain originally isolated from a rhesus monkey (BVrh). Here we report the genome sequence of a virulent BV strain isolated from a cynomolgus macaque (BVcy). The overall genome organization is the same, although sequence differences exist. The greatest sequence divergence is located in non-coding areas of the long and short repeat regions. Like BVrh, BVcy has duplicated Ori elements and lacks an ORF corresponding to the γ34.5 gene of herpes simplex virus. Nine of ten miRNAs and the majority of ORFs are conserved between BVrh and BVcy. The most divergent genes are several membrane-associated proteins and those encoding immediate early proteins. [ABSTRACT FROM AUTHOR]

Published

2014

3. Allogeneic cell stimulation enhances cytomegalovirus replication in the early period of primary infection in an experimental rat model

Author

Tamura, Kazuki, Oka, Tadayuki, Ohsawa, Kazutaka, Koji, Takehiko, Watanabe, Yoji, Katamine, Shigeru, Sato, Hiroshi, and Ayabe, Hiroyoshi

Subjects

*CYTOMEGALOVIRUS diseases, *HOMOGRAFTS, *COMPLICATIONS from organ transplantation

Abstract

: Background:Cytomegalovirus (CMV) diseases commonly occur in allograft recipients in the early post-transplant period. However, factors responsible for the high incidence of CMV diseases during this period are not yet fully defined.: Methods:Wistar–Furth (WF; RT-1u) rats were inoculated with 104 plaque-forming units (PFU) of rat CMV (RCMV) intraperitoneally, and then transplanted with allogeneic lungs from Dark Agouti (DA; RT-1avl) rats or stimulated with 107 mitomycin C–treated spleen cells from DA rats by daily sub-cutaneous injections for 2 weeks. No immunosuppressive agent was used. Naive WF rats and WF rats grafted with syngeneic lungs or cells were used as controls. The level of RCMV replication in rats was assessed by infectious virus titers in tissues.: Results:The virus titers in salivary glands of allogeneic and syngeneic lung graft recipients were significantly higher than in naive WF rats. The level of RCMV replication in rats stimulated with allogeneic spleen cells was significantly higher than in the syngeneic recipient rats: virus titers in the salivary gland of allogeneic and syngeneic recipients reached 4.61 ± 0.33 and 4.00 ± 0.37 log10 PFU/g tissue, respectively, at 14 days post-infection (p = 0.015). The augmented viral replication in allogeneic recipients was confirmed by an increase in the number of RCMV antigen–positive macrophages present in tissue sections of the salivary gland.: Conclusions:Acute lung allograft rejection and allogeneic spleen cell stimulation enhance CMV replication in the salivary gland of rats. Various responses to allogeneic antigens occurring in the process of acute allograft rejection could be risk factors for post-transplant CMV replication and infection. [Copyright &y& Elsevier]

Published

2003