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Characterization of the Recombinant Adenovirus Vector AdYB-1: Implications for Oncolytic Vector Development

机译:重组腺病毒载体AdYB-1的表征:溶瘤载体开发的意义。

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摘要

Conditionally replicating adenoviruses are a promising new modality for the treatment of cancer. However, early clinical trials demonstrate that the efficacy of current vectors is limited. Interestingly, DNA replication and production of viral particles do not always correlate with virus-mediated cell lysis and virus release depending on the vector utilized for infection. However, we have previously reported that nuclear accumulation of the human transcription factor YB-1 by regulating the adenoviral E2 late promoter facilitates viral DNA replication of E1-deleted adenovirus vectors which are widely used for cancer gene therapy. Here we report the promotion of virus-mediated cell killing as a new function of the human transcription factor YB-1. In contrast to the E1A-deleted vector dl312 the first-generation adenovirus vector AdYB-1, which overexpresses YB-1 under cytomegalovirus promoter control, led to necrosis-like cell death, virus production, and viral release after infection of A549 and U2OS tumor cell lines. Our data suggest that the integration of YB-1 in oncolytic adenoviruses is a promising strategy for developing oncolytic vectors with enhanced potency against different malignancies.
机译:有条件复制的腺病毒是治疗癌症的有希望的新形式。但是,早期的临床试验表明,当前载体的功效是有限的。有趣的是,取决于用于感染的载体,DNA复制和病毒颗粒的产生并不总是与病毒介导的细胞裂解和病毒释放相关。但是,我们以前曾报道过,通过调节腺病毒E2晚期启动子,人类转录因子YB-1的核积累促进了E1缺失的腺病毒载体的病毒DNA复制,该载体广泛用于癌症基因治疗。在这里,我们报告了病毒介导的细胞杀伤的促进作为人类转录因子YB-1的新功能。与缺失E1A的载体dl312相比,第一代腺病毒载体AdYB-1在巨细胞病毒启动子控制下过表达YB-1,导致感染A549和U2OS肿瘤后坏死样细胞死亡,病毒产生和病毒释放细胞系。我们的数据表明,YB-1在溶瘤腺病毒中的整合是开发具有增强的针对不同恶性肿瘤效力的溶瘤载体的有前途的策略。

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