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Titlebook: DNA Tumor Viruses; Oncogenic Mechanisms Giuseppe Barbanti-Brodano,Mauro Bendinelli,Herman Book 1995 Springer Science+Business Media New Yo

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Lecture Notes in Computer Sciencend monkeys and transform cells . to a neoplastic phenotype. For all these reasons, BKV and JCV have been considered possible candidates in the etiology of human tumors. Association of BKV, but not of JCV, with human tumors has been described, although a formal proof for an etiological role of BKV in
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Alla Menshikova,Daniil Kocharove.. In the past, although useful for basic studies, the SV40-induced hamster tumor model was considered to have only limited relevance in the elucidation of mechanisms for human cancer development. Recently, however, the discovery of relationships between SV40 proteins and human tumor suppressor gen
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Artificial Intelligence and Natural Languages that they all induce primarily benign proliferations of epithelial cells in their natural hosts. Individual members of this family show a high degree of both species specificity and tissue specificity. Squamous or mucosal epithelial cells are the targets of infection. The life cycle of the virus i
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Andrey Filchenkov,Lidia Pivovarova,Jan Žižkaural and biological properties. As many as five viruses associated with human hepatitis (the hepatitis A, B, C, D, and E viruses) have been isolated and fully characterized,. and the question of whether additional, uncharacterized viruses may be responsible for liver disease in some cases is still d
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Andrey Filchenkov,Lidia Pivovarova,Jan Žižka on entry into their host cells. Because these viruses have limited coding capacities, they cannot produce all of the protein products required to synthesize their new double-stranded DNA genomes and, therefore, must utilize many components of the host-cell machinery. In naturally occurring infectio
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