INHIBITION OF HUMAN OVARIAN-CANCER COLONY FORMATION BY ADRIAMYCIN AND ITS MAJOR METABOLITES
- 1 January 1980
- journal article
- research article
- Vol. 40 (11), 4109-4112
Abstract
The in vitro sensitivity to adriamycin of human ovarian cancer colonies cloned in soft agar was examined. In the 26 patients tested, 3 different patterns of sensitivity to adriamycin were observed. In 75% of the previously untreated patients, there was greater than 70% reduction in colony-forming cells after exposure to adriamycin (1.0 .mu.g/ml), a level which approximates the peak plasma level after i.v. therapy. In all the patients who had progressive disease while on a chemotherapy regimen without adriamycin, a greater than 70% reduction in colony-forming cells was observed only at a concentration of 10 .mu.g/ml, a level not achievable by i.v. administration. In 80% of patients with progressive disease after treatment with adriamycin as part of the primary chemotherapy regimen, a 70% reduction in tumor colony-forming cells could not be achieved even at 10 .mu.g/ml. These in vitro results are in agreement with clinical observations regarding the effectiveness of adriamycin in previously untreated patients (42% response rate) with ovarian cancer and its ineffectiveness (0-6% response rate) as a 2nd-line therapy in relapsed patients. The results also have provided a rationale for an ongoing Phase I trial of i.p. adriamycin in patients with ovarian cancer since cytotoxic levels can be produced i.p. using large-volume dialysis via a Tenckhoff dialysis catheter. The relative cytotoxicity of adriamycin to its 2 major metabolites, adriamycinol and adriamycin aglycone, was determined in the clonogenic assay. Both derivatives produced suppression of ovarian cancer colony formation; adriamycin was more cytotoxic than either metabolite.This publication has 11 references indexed in Scilit:
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