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Stability of gamma-glutamyltransferase activity in calf sera after refrigerated or frozen storage.
1997
Muller F. | Tyler J.W. | Parish S.M. | Johnson K.A. | Krytenberg D.S. | Wilson L.K.
Second-generation pseudorabies virus vaccine with deletions in thymidine kinase and glycoprotein genes.
1987
Kit S. | Sheppard M. | Ichimura H. | Kit M.
Efficacy of a pseudorabies virus vaccine based on deletion mutant strain 783 that does not express thymidine kinase and glycoprotein I.
1991
Oirschot J.T. van | Moormann R.J.M. | Berns A.J.M. | Gielkens A.L.J.
The vaccine efficacy of a genetically engineered deletion mutant strain of pseudorabies virus, strain 783, was compared with that of the conventionally attenuated Bartha strain. Strain 783 has deletions in the genes coding for glycoprotein I and thymidine kinase. In experiment 1, which had a 3-month interval between vaccination and challenge exposure, strain 783 protected pigs significantly (P < 0.05) better against virulent virus challenge exposure than did the Bartha strain. The growth of pigs vaccinated with strain 783 was not arrested, whereas that of pigs vaccinated with the Bartha strain was arrested for 7 days. Of 8 pigs given strain 783, 4 were fully protected against challenge exposure; none of the pigs given strain Bartha was fully protected. In experiment 2, which had a 3-week interval between vaccination and challenge exposure, the growth of pigs vaccinated with strain 783 was arrested for 3.5 days, whereas that of pigs vaccinated with the Bartha strain was arrested for 6 days. In experiment 3, pigs with moderate titer of maternal antibodies were vaccinated twice IM or once intranasally with either strain 783 or Bartha and were challenge-exposed 3 months after vaccination. Pigs given strain 783 twice IM were significantly (P < 0.05) better protected than were the other pigs. They had growth arrest of only 6 days, compared with 9 days for pigs of other groups, and shed less virus after challenge exposure. Results of this study indicate that the vaccine based on the deletion mutant strain 783 is more efficacious than is the Bartha strain of pseudorabies virus.
Afficher plus [+] Moins [-]Cytotoxic effect of acyclovir on cultured mammalian cells to which herpesvirus thymidine kinase gene was introduced
1989
Tanabe, K. (Hokkaido Univ., Sapporo (Japan). Faculty of Veterinary Medicine) | Hiraoka, W. | Kuwabara, M. | Sato, F. | Narita, T. | Niikura, M.
Studies on serum creatine phosphokinase isoenzyme: Seven cases of tetraplegia [paralysis of limbs due to spondylosis (spinal disease)] in the dog [for diagnosis of spinal disease]
1983
Yasuda, J. | Too, K. (Hokkaido Univ., Sapporo (Japan). Faculty of Veterinary Medicine)
Restriction fragment length polymorphism for the Yc subunit gene of rat liver glutathione S-transferase
1990
Sasaki, Y. (Hokkaido Univ., Sapporo (Japan). Faculty of Veterinary Medicine) | Hayashi, M. | Matsumoto, K. | Namioka, S.
Isolation of epithelial like cells from the rabbit myometrium; the distribution of creatine kinase and plasminogen activator
1984
Lee, C.W. (Kyongsang National Univ., Chinju (Korea R.)) | Iyengar, M.R. (Pennsylvania Univ. (USA). Dept of Veterinary Medicine)
Cells with an epithelioid morphology were isolated from the rabbit myometrium and were grown in culture. The cells had a doubling time of 53 hrs when grown in the presence of 10% fetal calf serum in Basal Eagle's medium with 3mM glutamine. In the presence of estrogen plus insulin, doubling time was reduced to 40 hrs. Creatine kinase activity upon reaching confluency was determined to be 0.019 uit per mg protein. Approximately 30% of the activity was extractable only in high ionic strength buffer. Cells also contained plasminogen activator with a specific activity of 140 CTA units per million cells
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