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- Title
Potential Utility of Bim<sub>S</sub> as a Novel Apoptotic Therapeutic Molecule
- Authors
Yip, Kenneth W.; Li, Anna; Li, Jian-Hua; Shi, Wei; Chia, Marie C.; Rashid, Shahnaz Al; Mocanu, Joseph D.; Louie, Alexander V.; Sanchez, Otto; Huang, Dolly; Busson, Pierre; Yeh, Wen-Chen; Gilbert, Ralph; O'sullivan, Brian; Gullane, Patrick; Liu, Fei-Fei
- Abstract
We have previously demonstrated a 1000-fold induction of gene expression exclusive to Epstein–Barr virus (EBV)-positive nasopharyngeal carcinoma (NPC) cells using an adenoviral vector (ad5.oriP). This platform allows us to explore tumor-specific gene therapy with BimS (ad5.oriP.BimS), a potent proapoptotic Bcl-2 family member. Ad5.oriP.BimS (25 infectious units (ifu)/cell) reduced C666-1 viability in a time- and dose-dependent manner to 15% survival. The effect was enhanced with radiation (6 Gy). Three days after infection, the proportion of apoptotic cells increased from 3.5% (control) to 47.5% (25 ifu/cell). Confocal microscopy demonstrated Bim colocalization to the mitochondria within 18 h of ad5.oriP.BimS infection. Ad5.oriP.BimS induced a 2.8-, 2.1-, and 1.85-fold increase in caspase-3, -8, and -9 activities, respectively. When C666-1 cells were infected with ad5.oriP.BimS (20 ifu/cell), no tumors formed in 7/9 mice followed for 100 days. Six intratumoral injections of ad5.oriP.BimS (1.5 × 109 ifu/dose) in combination with radiation were sufficient to cause almost complete disappearance of established C666-1 or C15 xenograft tumors. Intravenous injections of ad5.oriP.BimS (109 ifu) induced mild perturbation in liver function tests, associated with hepatocyte apoptoses and mitoses. This vector appears to be safe and effectively cytotoxic to EBV-positive NPC cells both in vitro and in vivo, mediated primarily through the induction of apoptosis.
- Subjects
CANCER; GENE therapy; ANTIGENS; APOPTOSIS
- Publication
Molecular Therapy, 2004, Vol 10, Issue 3, p533
- ISSN
1525-0016
- Publication type
Article
- DOI
10.1016/j.ymthe.2004.05.026