The levels of expression of
histocompatibility antigens on the cell membrane and their gene expression in non-metastatic and in highly metastatic Friend
leukemia cells (FLC) were measured and the levels of expression of these
antigens were correlated with the different in vivo behaviour of the
tumor cells. Highly metastatic in vivo passaged FLC (either
interferon-sensitive 745 or
interferon alpha/beta-resistant 3Cl-8 cells) expressed higher levels of class I H-2K and H-2D
antigens on their cell membrane with respect to the non-metastatic in vitro passaged counterparts. The increased expression of H-2
class I antigens was associated with an increased transcription of H-2K and H-2D genes. As both in vitro and in vivo passaged FLC have been shown to be resistant in vitro to the natural killer (NK) cell activity, we tried to correlate the levels of expression of
histocompatibility antigens with the in vivo clearance of [125I]UDR-labeled FLC. However, no correlation was found between the levels of expression of
H-2 antigens and the in vivo clearance of
tumor cells. In fact, in vivo passaged FLC (tested either after 1 or after 15 in vitro passages) expressed virtually identical levels of
H-2 antigens; however, the freshly explanted in vivo passaged FLC exhibited markedly lower levels of clearance from the lung, spleen and liver (when injected i.v. in DBA/2 mice) with respect to the corresponding FLC cultivated for several passages in vitro. Pretreatment of in vitro passaged 745 FLC with either
interferon alpha/beta or
interferon gamma resulted in the acquisition of some metastatic potential of FLC to the liver when
interferon-treated FLC were subsequently injected i.v. in DBA/2 mice; such in vitro treatments resulted in a 2-3-fold increase in the expression of H-2K
antigens versus the control untreated FLC. We suggest that such increases could represent some advantages for the homing properties of
tumor cells and/or for the
tumor progression, by mechanisms different from the resistance to the NK cells.