首页> 美国卫生研究院文献>Journal of Virology >Recombinant retroviruses that transduce middle T antigen cDNAs derived from polyomavirus mutants: separation of focus formation and soft-agar growth in transformation assays and correlations with kinase activities in vitro.
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Recombinant retroviruses that transduce middle T antigen cDNAs derived from polyomavirus mutants: separation of focus formation and soft-agar growth in transformation assays and correlations with kinase activities in vitro.

机译:转导自多瘤病毒突变体的中间T抗原cDNA的重组逆转录病毒:在转化分析中分离焦点形成和琼脂生长并与体外激酶活性相关。

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摘要

To study correlations between cellular transformation and the biochemical properties of polyomavirus middle T antigen, middle T cDNAs have been derived from the polyomavirus mutants dl1015, dl23, and NG59b and have been introduced into rodent fibroblast cell lines by using a retrovirus vector. It was found that all three mutants are completely defective in inducing growth in soft agar but possess a range of activities in assays of focus formation on cell monolayers. Furthermore, when assays of middle T antigen-associated kinase activities were performed in vitro, a correlation between the level of associated phosphatidylinositol kinase activity and the ability of mutant middle T antigens to induce focus formation was observed. However, the association of this activity with middle T antigen does not appear to be sufficient to bring about full transformation, since the middle T antigen derived from dl1015 is completely defective for soft-agar growth but is associated with a level of phosphatidylinositol kinase activity which is comparable to that of the wild type. Therefore, some other unidentified middle T antigen function may also be required for full transformation.
机译:为了研究细胞转化与多瘤病毒中间T抗原的生化特性之间的相关性,已从多瘤病毒突变体dl1015,dl23和NG59b衍生了中间T cDNA,并通过使用逆转录病毒载体将其引入了啮齿动物成纤维细胞系。已经发现,所有三个突变体在诱导软琼脂中的生长上都是完全缺陷的,但是在细胞单层上形成焦点的测定中具有一系列活性。此外,当在体外进行与中间T抗原相关的激酶活性的测定时,观察到相关磷脂酰肌醇激酶活性的水平与突变的中间T抗原诱导焦点形成的能力之间的相关性。但是,这种活性与中间T抗原的结合似乎不足以引起完全转化,因为衍生自dl1015的中间T抗原对于软琼脂的生长是完全有缺陷的,但是与磷脂酰肌醇激酶活性的水平有关。与野生型相当。因此,完全转化可能还需要一些其他未鉴定的中间T抗原功能。

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