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A retrogen plasmid-based vaccine generates high titer antibody responses against the autologous cancer antigen survivin and demonstrates anti-tumor efficacy.

Cancer letters 2006 Jun 8; 237(1):45-55

Link to PubMed abstract

Decker W WK, Qiu J J, Farhangfar F F, Hester J JH, Altieri D DC, Lin A AY

Department of Blood and Marrow Transplantation, The University of Texas MD Anderson Cancer Center, Box 65, 1515 Holcombe Blvd., Houston, TX 77030, USA. wkdecker@mdanderson.org

We describe the use of retrogen plasmid-based vaccine technology to break tolerance and to generate a robust, dose-dependent antibody response against the self cancer antigen, survivin. We further demonstrate that this phenomenon is due to the incorporation of the survivin antigen into the retrogen system rather than to some peculiarity unique to survivin. In contrast to other genetic immunization methods designed to produce antibody responses, the retrogen system results in a broad range of antibody isotypes, indicative of both a Th-1 and a Th-2 CD4+ response. Additional evidence of a Th-1 response is demonstrated by tumor growth inhibition in a mouse model of colon cancer metastasis. We speculate that this cost-effective technology could one day bolster or even supplant the use of monoclonal antibodies in the targeting of cell surface cancer antigens.