AUGMENTATION OF TUMOR-IMMUNITY AGAINST SYNGENEIC TUMORS IN MICE BY BETA-CAROTENE

Abstract

The effect of .beta.-carotene on tumor immunity was examined with the use of a syngeneic murine tumor system. Oral administration of .beta.-carotene (120 .mu.g/mouse/day) for 9 days from day 1 to the BALB/c mice inoculated sc with 107 syngeneic BALB/c Meth A fibrosarcoma cells (Meth A) led to a remarkable rejection against rechallenged Meth A implanted sc on day 10. The growth of Meth 1 fibrosarcoma (Meth 1), another syngeneic tumor of BALB/c origin, as a rechallenge tumor was unaffected by treatment with .beta.-carotene, thereby suggesting that .beta.-carotene may augment tumor rejection specific to tumor-specific antigens. Winn assay revealed that the suppressive effect on tumor growth of immune lymph node cells obtained from Meth A-inoculated .beta.-carotene-treated mice on day 12 was enhanced dose dependently. Primary effector cells responsible for the augmented rejection are Thy-1-positive, Lyt-1-negative, and Lyt-2-positive lymphocytes, presumably cytotoxic T-lymphocytes.