1. A CD46-binding Chimpanzee Adenovirus Vector as a Vaccine Carrier.
- Author
-
Tatsis, Nia, Blejer, Ariella, Lasaro, Marcio O., Hensley, Scott E., Cun, Ann, Tesema, Lello, Yan Li, Guang-Ping Gao, Xiang, Zhi Q., Dongming Zhou, Wilson, James M., and Ertl, Hildegund C. J.
- Subjects
- *
ADENOVIRUSES , *CHIMPANZEES , *GENETIC transduction , *GENETIC vectors , *TRANSGENIC animals , *GENE therapy - Abstract
A replication-defective chimeric vector based on the chimpanzee adenovirus serotype C1 was developed and tested as a vaccine carrier in mice. The AdC1 virus is closely related to human adenoviruses of subgroup B2 and uses CD46 for cell attachment. To overcome poor growth of E1-deleted AdC1 vectors on cell lines that provide the E1 of adenovirus of the human serotype 5 (AdHu5) virus in trans, the inverted terminal repeats and some of the early genes of AdC1 were replaced with those from AdC5, a chimpanzee origin adenovirus of subfamily E. The chimeric AdC1/C5 vector efficiently transduces CD46-expressing mouse dendritic cells (DCs) in vitro and initiates their maturation. Transduction of DCs in vivo is inefficient in CD46 transgenic mice. The AdC1/C5 vector induces transgene product-specific B- and CD8+ T-cell responses in mice. Responses are slightly higher in wild-type mice than in CD46 transgenic mice. Transgene product-specific T-cell responses elicited by the AdC1/C5 vector can be increased by priming or boosting with a heterologous adenovirus vector. Pre-existing immunity to adenovirus of the common human serotype 5 does not affect induction of cell-mediated immune responses by the AdC1/C5 vector. This vector provides an additional tool in a repertoire of adenovirus-based vaccine vectors.Molecular Therapy (2007) 15, 608–617. doi:10.1038/sj.mt.6300078; published online 16 January 2007 [ABSTRACT FROM AUTHOR]
- Published
- 2007
- Full Text
- View/download PDF