The arrest, retention, and elimination (i.e., clearance) of radiolabeled YAC-1
lymphoma cells injected either iv or into the left ventricle (LV) of the heart were studied in male BALB/c mice, with special emphasis on the role of natural killer (NK) cells. After iv injection YAC-1 cells were arrested and, to a large extent, destroyed in the lungs, which contain the first capillary bed that iv injected
tumor cells meet. After LV injection the initial distribution of the
tumor cells, which depends on the distribution of cardiac output at the time of injection, was estimated by use of radiolabeled
microspheres. Using this technique, we have shown that LV-injected
tumor cells, in contrast to iv injected
tumor cells, were not arrested in the first capillary bed that they encountered but passed viably through the microvasculature of the brain, heart, kidneys, intestinal tract, and to some extent, the bone, skin, and muscle. The only organs that could arrest the LV-injected
tumor cells were the lungs and the liver. In the lungs clearance of YAC-1 cells began immediately after the cells were arrested. However, the rate of clearance could be almost abrogated by pretreatment of the recipients with anti-
asialo GM1 antiserum, which destroys most of the NK cells in vivo and strongly depresses the in vitro NK cell activity. In contrast, YAC-1 cells arrested in the liver were not cleared from this organ during the first 1-2 hours after arrest. After this delay clearance of the cells commenced. Pretreatment of the recipients with anti-
asialo GM1 also strongly depressed the clearance of
tumor cells from the liver. Although pretreatment with
polyinosinic-polycytidylic acid enhanced in vitro NK cell activity, it could augment only slightly the clearance of YAC-1 cells from the lungs and the liver. Thus these results strongly support the hypothesis that the rapid clearance of
tumor cells from both the lungs and the liver depends, at least partially, on the NK cell activity within these organs.