Fig. 2.
NK-cell–mediated control of spontaneous metastasis by independent pfp and IFN-γ activities.
BALB/c, BALB/c.SCID, BALB/c.IFN-γ0, BALB/c.pfp0, and BALB/c pfp0.IFN-γ0 mice or BALB/c mice treated with anti-asialo GM1 antibody (100 μg/injection) were inoculated subcutaneously with DA3 tumor cells (105 or 5 × 105) as indicated. Mice depleted of subsets in vivo were treated on days −4, 0 (day of subcutaneous tumor inoculation), and weekly thereafter. Forty-two days after tumor inoculation, the lungs of these mice were harvested and fixed, and colonies were counted and recorded as the mean number of colonies ± SE. Asterisks indicate the groups that are significantly different from BALB/c-untreated mice (*P < .0001; **P < .005; Mann-Whitney U test). A significant difference was also detected between the BALB/c.P0 mice or BALB/c.IFN-γ0 mice and BALB/cP0.IFN-γ0 mice (P < .0001). The number of mice per group is shown in parentheses. Note that for groups of 5 mice receiving 105DA3 tumor cells, the numbers of DA3 lung colonies were as follows: BALB/c.B6Cmv1r = 8.0 ± 2.6; BALB/c.B6Cmv1r + anti-asialo GM1 antibody = 62.4 ± 6.6.