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Oncogenic activity of the BK type of human papova virus in inbred rat strains
Authors:G Noss  G Stauch  Prof J Drescher
Institution:(1) Institute of Virology, Medizinische Hochschule Hannover, Hannover-Kleefeld, Germany;(2) Institute of Pathology, Medizinische Hochschule Hannover, Hannover-Kleefeld, Germany;(3) Zentrum für Laboratoriumsmedizin, Institut für Virologie und Seuchenhygiene, Postfach 610180, D-3000 Hannover 1, Germany
Abstract:Summary The oncogenicity of the human polyomavirus BK (BKV) was tested in newborn inbred rats.It was found that the tumor rate was negatively correlated with the levels of T antibody 3 months after inoculation and the frequency of animals with detectable T antibodies 1.5 months after inoculation.By contrast, no influence of viral HI titers on the tumor rates was found. Thymectomy of animals resulted in most experiments in increased tumor rates. Inoculation with BKV of animals later than 24 hours after birth yielded a decrease of tumor rates.The results obtained suggest that T antibody titers present at a critical time after inoculation are associated with low oncogenicity of BKV.The oncogenicity of BKV was comparatively tested in rat strains possessing the allele ldquolrdquo or the allele ldquoardquo, respectively. The oncogenicity was significantly higher in rats with the allele ldquolrdquo than in rats with the allele ldquoardquo. Rats with the allele ldquolrdquo showed lower T antibody response than rats with the allele ldquoardquo.These differences could be explained by the finding that cells of ldquoardquo origin showedin vitro a higher percentage of T antigen bearing cells than did cells of a strain possessing the allele ldquolrdquo. In comparison to previous results obtained with BKV inoculated outbred WISTAR rats, the oncogenicity of comparable BKV doses in inbred rats was generally higher and the latency period of tumor manifestation shortened.
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