BCG-induced protection against malignant melanoma: Possible immunospecific effect in a murine system

Abstract

This report documents for the first time BCG-induced protection against a murine malignant melanoma. Adult Balb/C mice received 0.1-cm³ doses of BCG prior to intramuscular challenge with 1 × 10⁶ S-91 melanoma cells. A 65% reduction in melanoma incidence was noted in BCG-pretreated mice. The possibility of specific protection induced by the BCG against the melanoma exists, since the same BCG pretreatment did not protect against challenge with 1 × 10⁵ mammary carcinoma cells or 1 × 10⁴ MCA fibrosarcoma cells in the same strain of mice. Lack of immunogenicity was not a factor in the inability of the carcinoma and sarcoma to be inhibited by BCG. The strength of the BCG-induced protection against the S-91 melanoma was demonstrated by significantly decreased tumor incidence following three different log challenge doses of the melanoma. However, reduction of the sarcoma challenge dose to as few as 10² cells administered to BCG pretreated mice did not result in decreased tumor incidence. It was further discovered that as few as two doses of 0.1 cm³ of BCG were sufficient to produce a 70% reduction in melanoma incidence compared with the incidence in control animals (p <.001). Lymphocyte-mediated cytotoxicity studies paralleled the results of the in vivo experiments. Lymphocytes immune to each of the three tumors showed significant cytotoxicity against their respective tumor target cells (p <.001), while the only tumor cells that lymphocytes from BCG-pretreated mice showed significant cytotoxicity against were S-91 target cells (p <.01). Nonspecific cytotoxicity was not a factor in the effect of BCG-immune lymphocytes against S-91 target cells, since BCG-immune lymphocytes were not cytotoxic to Balb/C fibroblasts.