A Triad of Costimulatory Molecules Synergize to Amplify T‐‐Cell Activation in Both Vector‐‐Based and Vector‐‐Infected Dendritic Cell Vaccines
- 1 January 2003
- journal article
- Published by Taylor & Francis in Artificial Cells, Blood Substitutes, and Immobilization Biotechnology
- Vol. 31 (2) , 193-228
- https://doi.org/10.1081/bio-120020178
Abstract
The activation of a T cell has been shown to require two signals via molecules present on professional antigen presenting cells: signal 1, via a peptide//MHC complex, and signal 2, via a costimulatory molecule. Here, the role of three costimulatory molecules in the activation of T cells was examined. Poxvirus ((vaccinia and avipox)) vectors were employed because of their ability to efficiently express multiple genes. Murine cells provided with signal 1 and infected with either recombinant vaccinia or avipox vectors containing a TRIad of COstimulatory Molecules ((B7‐‐1//ICAM‐‐1//LFA‐‐3, designated TRICOM)) induced the activation of T cells to a far greater extent than cells infected with vectors expressing any one or two costimulatory molecules. Despite this T‐‐cell “hyperstimulation” using TRICOM vectors, no evidence of apoptosis above that seen using the B7‐‐1 vector was observed. Results employing the TRICOM vectors were most dramatic under conditions of either low levels of first signal or low stimulat...Keywords
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