Re-engineering adenovirus regulatory pathways to enhance oncolytic specificity and efficacy

被引:0
|
作者
Murali Ramachandra
Amena Rahman
Aihua Zou
Mei Vaillancourt
John A. Howe
Douglas Antelman
Barry Sugarman
G. William Demers
Heidrun Engler
Duane Johnson
Paul Shabram
机构
[1] Canji,
[2] Inc.,undefined
来源
Nature Biotechnology | 2001年 / 19卷
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摘要
Replicating adenoviruses may prove to be effective anticancer agents if they can be engineered to selectively destroy tumor cells. We have constructed a virus (01/PEME) containing a novel regulatory circuit in which p53-dependent expression of an antagonist of the E2F transcription factor inhibits viral replication in normal cells. In tumor cells, however, the combination of p53 pathway defects and deregulated E2F allows replication of 01/PEME at near wild-type levels. The re-engineered virus also showed significantly enhanced efficacy compared with extensively studied E1b-deleted viruses such as dl1520 in human xenograft tumor models.
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页码:1035 / 1041
页数:6
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