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p53 promotes adenoviral replication and increases late viral gene expression

机译:p53促进腺病毒复制并增加晚期病毒基因表达

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摘要

The tumor suppressor protein, p53, plays a critical role in viro-oncology. However, the role of p53 in adenoviral replication is still poorly understood. In this paper, we have explored further the effect of p53 on adenoviral replicative lysis. Using well-characterized cells expressing a functional p53 (A549, K1neo, RKO) and isogenic derivatives that do not (K1scx, RKOp53.13), we show that virus replication, late virus protein expression and both wtAd5 and ONYX-015 virus-induced cell death are impaired in cells deficient in functional p53. Conversely, by transfecting p53 into these and other cells (IIICF/c, HeLa), we increase late virus protein expression and virus yield. We also show, using reporter assays in IIICF/c, HeLa and K1scx cells, that p53 can cooperate with E1a to enhance transcription from the major late promoter of the virus. Late viral protein production is enhanced by exogenous p53. Taken together, our data suggest that functional p53 can promote the adenovirus (Ad) lytic cycle. These results have implications for the use of Ad mutants that are defective in p53 degradation, such as ONYX-015, as agents for the treatment of cancers.
机译:肿瘤抑制蛋白p53在病毒肿瘤学中起着至关重要的作用。但是,p53在腺病毒复制中的作用仍然知之甚少。在本文中,我们进一步探讨了p53对腺病毒复制裂解的作用。使用表达良好的功能性细胞表达功能性p53(A549,K1neo,RKO)和等基因衍生物不表达的细胞(K1scx,RKOp53.13),我们显示病毒复制,晚期病毒蛋白表达以及wtAd5和ONYX-015病毒诱导在缺乏功能性p53的细胞中,细胞死亡受到损害。相反,通过将p53转染到这些细胞和其他细胞(IIICF / c,HeLa)中,我们可以提高后期病毒蛋白的表达和病毒产量。我们还显示,使用IIICF / c,HeLa和K1scx细胞中的报告基因分析,p53可以与E1a协同增强从病毒主要晚期启动子的转录。后期病毒蛋白的产生可通过外源性p53增强。两者合计,我们的数据表明功能性p53可以促进腺病毒(Ad)裂解周期。这些结果暗示了使用p53降解缺陷的Ad突变体,例如ONYX-015,作为癌症的治疗剂。

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