Abstract
Resistance to cytotoxic chemotherapy is a major problem in the management of patients with metastatic breast cancer. Various data suggest P-glycoprotein-associated multidrug resistance (MDR) to be a relevant resistance mechanism in this tumor. The purpose of this study was to evaluate feasibility and activity of combining oral dexverapamil, a second-generation chemosensitizer currently in clinical development for MDR reversal, with epirubicin in patients with epirubicin-refractory high-risk metastatic breast cancer. Patients first received epirubicin alone at 120 mg/m2. In cases of clinical refractoriness, epirubicin was continued at the same dose and schedule but supplemented with oral dexverapamil. Dexverapamil was given at 300 mg every 6 h for a total of 13 doses and commenced 2 days prior to epirubicin administration. At the time of this interim analysis, 41 patients had received epirubicin alone and 20 proceeded to treatment with epirubicin plus dexverapamil. Of the 20 patients, 14 were considered evaluable for toxicity and activity. Addition of dexverapamil resulted in a significant decrease in mean heart rate and blood pressure as well as prolongation of PQ time as compared to epirubicin alone. However, these cardiovascular effects of dexverapamil were usually mild, and subjective tolerance of treatment was good. In 7/14 patients, dose escalation of dexverapamil was feasible. Dexverapamil had no effect on epirubicin toxicities and did not require reduction of the epirubicin dose. In 2/14 patients, the addition of dexverapamil to epirubicin was able to convert progressive disease and no changes respectively, into partial responses. In 3 patients with progressive disease, addition of dexverapamil temporarily prevented further tumor progression. Analyses of dexverapamil and nor-dexverapamil plasma levels, of in vitro reversal activity of patient sera containing dexverapamil, and of epirubicin pharmacokinetics without and with dexverapamil are currently in progress. Addition of oral dexverapamil to epirubicin 120 mg/m2 proved to be feasible in a multiinstitutional setting. Patient accrual is continuing to determine whether dexverapamil is capable of overcoming epirubicin refractoriness in a significant number of patients with metastatic breast cancer.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Echizen H, Brecht T, Niedergesaess, S, Vogelsang B, Eichelbaum M (1985) The effect of dextro-levo- and racemic verapamil on atrio-ventricular conduction in humans. Am Heart J 109:210–217
Endicott JA, Ling V (1989) The biochemistry of P-glycoprotein mediated multidrug resistance. Annu Rev Biochem 58:137–171
Ford JM, Hait WN (1990) Pharmacology of drugs that alter multidrug resistance in cancer. Pharmacol Rev 42:155–199
Gehan EA, Schneiderman MA (1982) Experimental design of clinical trials. In: Holland JF, Frei E III (eds) Cancer medicine, 2nd edn. Lea & Febiger, Philadelphia, pp 531–553
Gotesmann MM, Pastan I (1993) Biochemistry of multidrug resistance mediated by the multidrug transporter. Annu Rev Biochem 62:385–427
Gruber A, Peterson C, Reizenstein P (1988)d-Verapamil andl-verapamil are equally effective in increasing vincristine accumulation in leukemic cells in vitro. Int J Cancer 41:224–226
Hayward JL, Carbone PP, Heuson JC, Rubens RD, Kumaoka S, Segaloff A (1977) Assessment of response to therapy in advanced breast cancer. Eur J Cancer 13:89–94
Lehnert M (1993) Reversal of multidrug resistance in breast cancer: many more open questions than answers. Ann Oncol 4:11–13
Lehnert M (1994) Reversal of P-glycoprotein-associated multidrug resistance: from bench to bedside. Onkologie 17:8–15
Lum BL, Kraubisch S, Yahanda AM, Adler KM, Jew L, Ehsan NN, Brophy NA, Halsey J, Gosland MP, Sikic BI (1992) Alteration of etoposide pharmacokinetics and pharmacodynamics by cyclosporine in a phase I trial to modulate multidrug resistance. J Clin Oncol 10:1635–1642
Marschner N, Kreienberg R, Souchon R, Räth U, Eggeling B, Voigtmann R, Ruffert K, Schütte M, Ammon A, Kesztyüs T, Kaplan E, Nagel G (1994) Evaluation of the importance and relevance of dose intensity using epirubicin and cyclosphosphamide in metastatic breast cancer: interim analysis of a prospective randomized trial. Semin Oncol 21 [Suppl 1]:10–16
Mickisch GH, Kössig J, Keilhauer G, Schlick E, Tschada RK, Alken PM (1990) Effects of calcium antagonists in multidrug resistant primary human renal cell carcinomas. Cancer Res 50:3670–3674
Miller AB, Hoogstraten B, Staquet M, Winkler A (1981) Reporting results of cancer treatment. Cancer 47:207–214
Miller TP, Grogan TM, Dalton WS, Spier CM, Scheper RS, Salmon SE (1991) P-glycoprotein expression in malignant lymphoma and reversal of clinical drug resistance with chemotherapy plus high-dose verapamil. J Clin Oncol 9:17–24
Moscow JA, Cowan KH (1988) Multidrug resistance. J Natl Cancer Inst 80:14–20
Mross K, Hamm K, Hossfeld DK (1993a) Effects of verapamil on the pharmacokinetics and metabolism of epirubicin. Cancer Chemother Pharmacol 31:369–375
Mross K, Bohn C, Edler L, Jonat W, Queisser W, Heidemann E, Goebel M, Hossfeld DK (1993b) Randomized phase II study of single-agent epirubicin +/- verapamil in patients with advanced metastatic breast cancer. Ann Oncol 4:45–50
Pirker R, Keilhauer G, Raschak M, Lechner C, Ludwig H (1990) Reversal of multi-drug resistance in human KB cell lines by structural analogs of verapamil. Int J Cancer 45:916–919
Salmon SE, Dalton WS, Grogan TM, Plezia P, Lehnert M, Roe DJ, Miller TP (1991) Multidrug resistant myeloma: laboratory and clinical effects of verapamil as a chemosensitizer. Blood 78:44–50
Scheithauer W, Schenk T, Czejka M (1993) Pharmacokinetic interaction between epirubicin and the multidrug resistance reverting agent d-verapamil. Br J Cancer 68:8–9
Tsuruo T, Lida H, Tsukagoshi S, Sakura Y (1981) Overcoming of vincristine resistance in P388 leukemia in vivo and in vitro through enhanced cytotoxicity of vincristine and vinblastine by verapamil. Cancer Res 41:1967–1972
Verrelle P, Meissonier F, Fonck Y, Feillel V, Dionet C, Kwiatkowski F, Plagne R, Chassagne J (1991) Clinical relevance of immunohistochemical detection of multidrug resistance P-glycoprotein in breast carcinoma. J Natl Cancer Inst 83:111–116
Author information
Authors and Affiliations
Rights and permissions
About this article
Cite this article
Thürlimann, B., Kröger, N., Greiner, J. et al. Dexverapamil to overcome epirubicin resistance in advanced breast cancer. J Cancer Res Clin Oncol 121 (Suppl 3), R3–R6 (1995). https://doi.org/10.1007/BF02351063
Issue Date:
DOI: https://doi.org/10.1007/BF02351063