Mice carrying large established major histocompatibility complex (MHC) class 1+ sarcoma tumors can be successfully treated by immunization with genetically engineered sarcoma cells transfected with syngeneic MHC class II plus B7-1 genes. This approach is significantly more effective than previously described strategies using cytokine- or B7-transduced tumor cells which are only effective against smaller tumor loads, and which cannot mediate regression of longer-term established tumors. The most efficient tumor rejection occurs if both the class II and B7-1 molecules are coexpressed on the same tumor cell. Immunity induced by immunization with class II+B7-1(+)-transfected sarcoma cells involves CD4+ and CD8+ T cells, suggesting that the increased effectiveness of the transfectants is due to their ability to activate both of these T cell populations.
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1 February 1995
Article|
February 01 1995
Major histocompatibility complex class II+B7-1+ tumor cells are potent vaccines for stimulating tumor rejection in tumor-bearing mice.
S Baskar,
S Baskar
Department of Biological Sciences, University of Maryland, Baltimore 21228.
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L Glimcher,
L Glimcher
Department of Biological Sciences, University of Maryland, Baltimore 21228.
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N Nabavi,
N Nabavi
Department of Biological Sciences, University of Maryland, Baltimore 21228.
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R T Jones,
R T Jones
Department of Biological Sciences, University of Maryland, Baltimore 21228.
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S Ostrand-Rosenberg
S Ostrand-Rosenberg
Department of Biological Sciences, University of Maryland, Baltimore 21228.
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S Baskar
,
L Glimcher
,
N Nabavi
,
R T Jones
,
S Ostrand-Rosenberg
Department of Biological Sciences, University of Maryland, Baltimore 21228.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1995) 181 (2): 619–629.
Citation
S Baskar, L Glimcher, N Nabavi, R T Jones, S Ostrand-Rosenberg; Major histocompatibility complex class II+B7-1+ tumor cells are potent vaccines for stimulating tumor rejection in tumor-bearing mice.. J Exp Med 1 February 1995; 181 (2): 619–629. doi: https://doi.org/10.1084/jem.181.2.619
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