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多瘤病毒基因型与小鼠肿瘤诱导的关系。具有广泛不同肿瘤特征的野生型菌株的特征。

Variations in polyoma virus genotype in relation to tumor induction in mice. Characterization of wild type strains with widely differing tumor profiles.

作者信息

Dawe C J, Freund R, Mandel G, Ballmer-Hofer K, Talmage D A, Benjamin T L

出版信息

Am J Pathol. 1987 May;127(2):243-61.

Abstract

The authors have explored the effects of variations in mouse polyoma virus genotype on patterns of tumor formation in the mouse. Four "wild type" virus strains were surveyed. Two were highly oncogenic, inducing multiple tumors of epithelial and mesenchymal origin, at high frequency and with short latency. The other two strains were weakly oncogenic, inducing fewer tumors, solely of mesenchymal origin, and after a long latency. These sharply contrasting tumor profiles were reproduced with virus stocks derived from molecularly cloned viral genomes. Though vastly different in their oncogenic properties, these cloned viruses proved equally effective in transforming established rat fibroblasts in culture and showed the same patterns of tumor antigen expression in cultured mouse cells. Complexes of polyoma middle T antigen and pp60c-src were demonstrated in extracts of epithelial tumors induced by a highly oncogenic virus strain. It is concluded that polyoma viral genetic determinants for tumor induction in the mouse are more complex than those previously defined by the use of cell transformation systems.

摘要

作者们探究了小鼠多瘤病毒基因型的变化对小鼠肿瘤形成模式的影响。研究了四种“野生型”病毒株。其中两种具有高度致癌性,能高频且短潜伏期地诱导产生多种上皮和间充质来源的肿瘤。另外两种病毒株致癌性较弱,仅诱导产生较少的、间充质来源的肿瘤,且潜伏期较长。这些截然不同的肿瘤特征在用分子克隆的病毒基因组衍生的病毒株中得到了重现。尽管这些克隆病毒的致癌特性差异巨大,但它们在体外转化已建立的大鼠成纤维细胞方面同样有效,并且在培养的小鼠细胞中显示出相同的肿瘤抗原表达模式。在一种高度致癌病毒株诱导的上皮肿瘤提取物中证实了多瘤病毒中T抗原与pp60c-src的复合物。得出的结论是,小鼠中多瘤病毒诱导肿瘤的遗传决定因素比以前通过细胞转化系统所定义的更为复杂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f2e2/1899751/7c945c814f72/amjpathol00146-0058-a.jpg

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