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条件复制型腺病毒对 p53 转录功能失调的靶向作用不受 p53 同源物的限制。

Targeting of p53-transcriptional dysfunction by conditionally replicating adenovirus is not limited by p53-homologues.

机构信息

Department of Gastroenterology, Hepatology and Endocrinology, Medical School Hannover, Hannover, Germany.

出版信息

Mol Ther. 2010 May;18(5):936-46. doi: 10.1038/mt.2009.298. Epub 2009 Dec 29.

Abstract

A hallmark of human tumors is the loss of p53 or its transcriptional functions. In this study, we describe the generation of the conditionally replicating adenovirus Adp53sensor for the treatment of p53-dysfunctional tumors. p53-selective attenuation of viral replication was achieved by using p53-dependent expression of the transcriptional repressor Gal4-KRAB that was directed against the adenoviral E1A locus. Adp53sensor shows efficient replication in p53-dysfunctional, but not in p53-active cells. In p53-dysfunctional cells, p53-analogous transcriptional activity by other p53 family members was not sufficient to compromise replication of Adp53sensor. In comparison with a genetically similar, but p53-insensitive virus, Adp53sensor replication was inhibited after systemic infection of p53-wt-mice, but not in p53-ko-mice thus confirming the correct function of the chosen approach. Adp53sensor showed efficient lytic and replicative properties in all investigated cells with p53-dysfunction and successfully inhibited the growth of subcutaneous xenotransplants in vivo. We further demonstrated that intravenous injection of Adp53sensor lead to significantly reduced liver damage compared to the control virus. Together, our data show that Adp53sensor is an oncolytic, p53-selective adenovirus for efficient treatment of p53-dysfunctional tumors with a favorable toxicity profile. Moreover, Adp53sensor provides a strategy that should be applicable to other transcriptionally regulated DNA viruses.

摘要

人类肿瘤的一个特征是 p53 或其转录功能的丧失。在这项研究中,我们描述了条件复制腺病毒 Adp53sensor 的产生,用于治疗 p53 功能失调的肿瘤。通过使用依赖于 p53 的转录抑制剂 Gal4-KRAB 的表达来实现病毒复制的 p53 选择性衰减,该抑制剂针对腺病毒 E1A 基因座。Adp53sensor 在 p53 功能失调的细胞中显示出有效的复制,但在 p53 活跃的细胞中则不行。在 p53 功能失调的细胞中,其他 p53 家族成员的 p53 类似转录活性不足以损害 Adp53sensor 的复制。与遗传上相似但对 p53 不敏感的病毒相比,Adp53sensor 在 p53-wt 小鼠的全身感染后被抑制复制,但在 p53-ko 小鼠中则没有,从而证实了所选择方法的正确功能。Adp53sensor 在所有研究的具有 p53 功能失调的细胞中均显示出有效的溶细胞和复制特性,并成功抑制了体内异种移植肿瘤的生长。我们进一步证明,与对照病毒相比,Adp53sensor 的静脉注射导致肝损伤明显减少。总之,我们的数据表明,Adp53sensor 是一种溶瘤、p53 选择性腺病毒,可有效治疗 p53 功能失调的肿瘤,且具有良好的毒性特征。此外,Adp53sensor 提供了一种策略,该策略应该适用于其他转录调控的 DNA 病毒。

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