Inhibition of PKCα decreases the gelatinase activity and the angiogenic and metastatic ability of the highly metastatic B16 murine melanoma cells

We have examined the concept of genomic instability in relation to the metastatic progression of low ( F I ) and high metastasis (BL6, ML8) clones of the 61 6 mouse melanoma, by using a mutation assay, and DNA strand break repair and repair fidelity assays. The frequency of induced ouabain resistant

## Abstract We have examined the influence of fibroblasts on the invasive and migratory potential of highly metastatic melanoma B16‐BL6 and weakly metastatic B16‐FI cells __in vitro.__ Co‐culture of B16‐BL6 cells with a fibroblast monolayer without cellular contact in a Transwell chamber more effec

The synthetic matrix metalloproteinase inhibitor batimastat was tested for its ability to inhibit growth and metastatic spread of the B16-BL6 murine melanoma in syngeneic C57BL/6N mice. lntraperitoneal administration of batimastat resulted in a significant inhibition in the number of lung colonies p

The H-Zb-negative B78H I clone (derived from B 16 melanoma) was transfected with the H-2Kb gene; 4 cell clones expressing membrane H-2Kb antigens and 2 control clones (transfected with pSV,neo alone) were used for studies of metastatic ability, immunogenicity, N K sensitivity and homotypic adhesion.