Summary Mice transplanted with NC carcinoma were treated with the thromboxane synthetase inhibitor dazmegrel (UK38485) or with nafazatrom (BAY G 6575), a compound that is reported to increase prostacyclin formation. Some experiments included the cytotoxic drugs methotrexate and melphalan. The tumours were excised under anaesthesia on day 14 or day 21 after transplanation, and weighed; some were extracted for prostanoids which were measured by radioimmunoassay. Mouse survival time was determined up to day 121, and cancer spread was determined by postmortem examination. The survival was increased by methotrexate and melphalan but not by the other drugs. Nafazatrom-treated mice tended to have lighter tumours. Although dazmegrel reduced the formation of thromboxane B2 during clotting of blood from normal mice, it did not affect the tumour yields of prostanoids. Nafazatrom had no effect on serum or tumour prostanoids. There were no obvious effects of the treatments on the recurrence of tumour in the excision scar, lung metastasis or spread to lymph nodes.Effects of the arachidonate metabolites thromboxane A2 (TXA2) and prostacyclin (PGI2) on platelet aggregation are well known. The ability of TXA2 produced by platelets to cause their aggregation may normally be balanced by PGI2 which is inhibitory (Moncada & Vane, 1979). Platelet aggregation is thought to be important in the haematogenous spread of some tumours, and Honn (1982) and his colleagues (Honn et al., 1981(Honn et al., , 1983 suggested that circulating tumour cells, or vesicles shed from the primary tumour cells, disrupt the balance between PGI2 and TXA2 in favour of platelet aggregation. Experiments with intravenously injected B-16a melanoma cells showed that thromboxane synthesis inhibitors, PGI2, or nafazatrom (which has various actions including an increase of PGI2 formation), are antimetastatic (Honn, 1982;Honn et al., 1983). A thromboxane synthesis inhibitor also reduced spontaneous metastasis from Lewis lung carcinoma (Honn, 1982 Drugs that inhibit cyclo-oxygenase usually reduce the size of NC tumours, and prolong host survival when given alone or with the cytotoxic drugs methotrexate and melphalan (Bennett et al., 1979(Bennett et al., , 1982. Cyclo-oxygenase inhibitors reduce both thromboxane and prostaglandin formation, but it is not known if the effect on thromboxane production contributes to the effects of indomethacin and flurbiprofen on tumour size and mouse survival.The aims of the present study were: (i) to examine Honn's hypothesis, using nafazatrom or the thromboxane synthetase inhibitor dazmegrel in the mouse NC tumour model, (ii) to measure mouse survival time, tumour weight and prostanoid content and (iii) to study the effect of dazmegrel in combination with cytotoxic drugs.
Materials and methodsThe NC carcinoma used in these studies originally arose spontaneously in the mammary region of a WHT/Ht mouse (Hewitt et al., 1976), the same strain used in our experiments. Following local excision of this carcinoma there is a high incidence of l...
