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*Compound via MeSH
*Substance via MeSH
Hazardous Substances DB
*MELPHALAN
*MITOMYCIN C
The Journal of Immunology, 2000, 164: 6230-6236.
Copyright © 2000 by The American Association of Immunologists

Melphalan and Other Anticancer Modalities Up-Regulate B7-1 Gene Expression in Tumor Cells1

Dorothy K. Sojka*, Manjula Donepudi*, Jeffrey A. Bluestone2,{dagger} and Margalit B. Mokyr2,3,*

* Department of Biochemistry and Molecular Biology, University of Illinois, Chicago, IL 60612; and {dagger} The Ben May Institute for Cancer Research, Committee on Immunology, and Department of Pathology, University of Chicago, Chicago, IL 60637

In this study, we show that administration of low-dose melphalan (L-PAM, L-phenylalanine mustard) to mice bearing a large MOPC-315 plasmacytoma led to a rapid up-regulation of B7-1 (CD80), but not B7-2 (CD86), expression on the surface of MOPC-315 tumor cells. This L-PAM-induced preferential up-regulation of B7-1 surface expression was due, at least in part, to a direct effect of L-PAM on the tumor cells, as in vitro exposure of MOPC-315 tumor cells to L-PAM led to the preferential up-regulation of B7-1 surface expression. Moreover, in vitro exposure of MOPC-315 tumor cells to two other anticancer modalities, {gamma}-irradiation and mitomycin C, resulted in the preferential up-regulation of B7-1 surface expression. This effect was not restricted to MOPC-315 tumor cells, as preferential up-regulation of B7-1 surface expression was observed also following in vitro exposure of the P815 mastocytoma (that is negative for both B7-1 and B7-2 surface expression) to any of the three anticancer modalities. The up-regulation of B7-1 surface expression following in vitro exposure of tumor cells to L-PAM, {gamma}-irradiation, or mitomycin C required de novo protein and RNA synthesis, and was associated with the accumulation of mRNA for B7-1 within 4–8 h, indicating that the regulation of B7-1 expression is at the RNA transcriptional level. These results have important implications for an additional immune-potentiating mechanism of these anticancer modalities in clinical setting.




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