Origin and evolution of the c-src-transducing avian sarcoma virus PR2257

生物 病毒学 病毒 原癌基因酪氨酸蛋白激酶Src 肉瘤 遗传学 病理 激酶 医学
作者
Bogdan Yatsula,J Geryk,J. Briestanska,I Karakoz,Jan Svoboda,A. V. Rynditch,Georges Calothy,Philippe Dezélée
出处
期刊:Journal of General Virology [Microbiology Society]
卷期号:75 (10): 2777-2781 被引量:10
标识
DOI:10.1099/0022-1317-75-10-2777
摘要

Avian sarcoma virus PR2257 transduced de novo the c- src gene and about 900 bp of 3‣ non-coding sequences belonging to the src locus. This virus contains only one mutation in the c-src coding sequence causing a reading frame shift after Pro-525. The molecular clone studied was derived from a cell line of transformed quail fibroblasts, Cl. It contains endogenous virus (ev) derived sequences in the U5 and 3‣ non-coding regions, indicating that multiple recombination occurred with endogenous virus. Here we investigated the possible evolution of PR2257 when the original tumour was repeatedly passaged in vivo. After 16 passages a new virus, designated PR2257/16, appeared with a tenfold higher titre. The sequence ofPR2257/16 was determined and showed that PR2257/16 resulted from recombination of PR2257 with the env gene of the helper virus (td daPR-C) This recombination expanded the env gene content in PR2257/16 and, in addition, five point mutations occurred in its genome. Because we thought that an endogenous virus might be involved in the mechanism of c-src transduction, we also reinvestigated the presence of ev sequences in PR2257 proviruses from several early passages of the original tumour. We found that in contrast with the first isolate from the C7 cell line, the provirus in these tumours did not contain such sequences. These results do not support the hypothesis that endogenous sequences were involved in the transduction process.
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