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Polyoma viral middle T-antigen is required for transformation.

机译:转化需要PolyoMa病毒中间T-抗原。

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To determine whether small or middle T-antigen (or both) of polyoma virus is required for transformation, we constructed mutants of recombinant plasmids which bear the viral oncogene and measured the capacity of these mutants to transform rat cells in culture. Insertion and deletion mutations in sequences encoding small and middle T-antigens (79.7, 81.3, and 82.9 map units) rendered the DNA incapable of causing transformation by the focus assay. Similar mutations in sequences that encoded middle but not small T-antigen (89.7, 92.1, and 96.5 map units) generally abolished the transforming activity of the DNA. However, two mutants (pPdl1-4 and PPd12-7) that carried deletions at 92.1 map units retained the capacity to transform cells; pPdl1-4 did so at frequencies equal to those of the parental plasmid, whereas pPdl2-7 transformed at 10% the frequency of its antecedent. From these studies we conclude that small T-antigen alone is insufficient to cause transformation and that middle T-antigen is required for transformation, either in combination with small T-antigen or by itself.
机译:为了确定转化所需的多瘤病毒是否小或中间T-抗原(或两者),我们构成了具有病毒癌基因的重组质粒的突变体,并测量了这些突变体在培养中转化大鼠细胞的能力。编码小和中间T抗原的序列中的插入和缺失突变(79.7,81.3和82.9个地图单元)使DNA不能通过聚焦测定导致转化。编码中间但不小的T-抗原(89.7,92.1和96.5映射单元)的类似突变通常废除了DNA的转化活性。然而,在92.1映射单元以92.1映射单元递送缺失的两个突变体(PPDL1-4和PPD12-7)保留了转化细胞的能力; PPDL1-4在等于亲本质粒的频率下以频率为单位,而PPDL2-7以10%转化为10%的频率。从这些研究中,我们得出结论,单独的小T-抗原不足以导致转化,并且中间T-抗原是转化的,或者与小T-抗原或本身组合。

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