Randomized phase III trial comparing the new potent and selective third-generation aromatase inhibitor vorozole with megestrol acetate in postmenopausal advanced breast cancer patients. North American Vorozole Study Group.

PURPOSE To compare the efficacy and safety of vorozole (VOR) 2.5 mg once daily with that of megestrol acetate (MA) 40 mg four times per day as second-line therapy in postmenopausal women with advanced breast cancer whose disease progressed after tamoxifen treatment. PATIENTS AND METHODS A total of 452 patients were enrolled onto an open, multicenter, randomized phase III trial comparing VOR to MA for tumor response, safety, and quality of life (as indicated by the Functional Living Index-Cancer score). RESULTS Vorozole produced a response rate of 9.7%, compared with 6.8% for MA (P = .24). Clinical benefit (complete response + partial response + no change in > 6 months) was demonstrated in 23.5% and 27.2% of patients treated with VOR and MA, respectively (P = .42). Median duration of response was 18.2 months for VOR versus 12.5 months for MA (P = .074). There was no significant difference in time to progression or survival between the treatment groups. Discontinuation of treatment because of adverse events occurred less frequently in the VOR-treated group (3.1% v 6.2%; P = .18). Patients on the VOR arm reported significantly more nausea, hot flushes, arthralgia, upper respiratory tract infection, anorexia, and paresthesia, whereas those treated with MA had significantly more dyspnea, increased appetite, and weight increase. There was no difference between the two treatment groups in Functional Living Index-Cancer scores (total or subscales). However, when analyzed by objective response, patients with complete or partial responses (P = .032) or no change (P = .033) who were receiving VOR had significant improvement in the psychologic well-being subscale, compared with patients given MA. CONCLUSION Vorozole is well tolerated and as effective as MA in the treatment of postmenopausal advanced breast cancer patients with disease progression after tamoxifen treatment.

[1]  S. Dahrouge,et al.  Comparison of antiestrogen and progestogen therapy for initial treatment and consequences of their combination for second-line treatment of recurrent breast cancer. , 1990, Seminars in oncology.

[2]  J. Gockerman,et al.  Randomized comparison of tamoxifen versus diethylstilbestrol in estrogen receptor-positive or -unknown metastatic breast cancer: a Southeastern Cancer Study Group trial. , 1986, Cancer treatment reports.

[3]  A Howell,et al.  Anastrozole, a potent and selective aromatase inhibitor, versus megestrol acetate in postmenopausal women with advanced breast cancer: results of overview analysis of two phase III trials. Arimidex Study Group. , 1996, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[4]  H. Mouridsen,et al.  Tamoxifen in advanced breast cancer. , 1978, Cancer treatment reviews.

[5]  P. Siiteri,et al.  Plasma precursors of estrogen. II. Correlation of the extent of conversion of plasma androstenedione to estrone with age. , 1974, The Journal of clinical endocrinology and metabolism.

[6]  M. Williams,et al.  Factors predicting the response of patients with advanced breast cancer to endocrine (Megace) therapy. , 1989, European journal of cancer & clinical oncology.

[7]  A McMurray,et al.  Measuring the quality of life of cancer patients: the Functional Living Index-Cancer: development and validation. , 1984, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[8]  D. Osoba,et al.  The EORTC Core Quality-of-Life Questionnaire: Interim Results of an International Field Study * , 2021, Effect of Cancer on Quality of Life.

[9]  J. de Haes,et al.  Measuring psychological and physical distress in cancer patients: structure and application of the Rotterdam Symptom Checklist. , 1990, British Journal of Cancer.

[10]  D. Sleijfer,et al.  A randomized comparison of megestrol acetate (MA) and medroxyprogesterone acetate (MPA) in patients with advanced breast cancer. , 1990, European journal of cancer.

[11]  D. Schoenfeld,et al.  Sample-size formula for the proportional-hazards regression model. , 1983, Biometrics.

[12]  M. Dowsett,et al.  Clinical and endocrine effects of the oral aromatase inhibitor vorozole in postmenopausal patients with advanced breast cancer. , 1994, Cancer research.

[13]  J. Haybittle,et al.  A randomised trial of second-line hormone vs single agent chemotherapy in tamoxifen resistant advanced breast cancer. , 1992, British Journal of Cancer.

[14]  R. Pichlmayr,et al.  Strategies in the surgical treatment of gastric carcinoma. , 1994, Annals of oncology : official journal of the European Society for Medical Oncology.

[15]  David R. Cox,et al.  Regression models and life tables (with discussion , 1972 .

[16]  I. Tannock,et al.  Criteria of tumor response used in clinical trials of chemotherapy. , 1985, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[17]  W. Miller Aromatase inhibitors in the treatment of advanced breast cancer. , 1989, Cancer treatment reviews.

[18]  M. Espié Megestrol acetate in advanced breast carcinoma. , 1994, Oncology.

[19]  Jordan Vc Tamoxifen for breast cancer prevention , 1995 .

[20]  J. Ingle,et al.  Randomized clinical trial of megestrol acetate versus tamoxifen in paramenopausal or castrated women with advanced breast cancer. , 1982, American journal of clinical oncology.

[21]  J. Garcia-conde,et al.  Aromatase activity and estradiol in human breast cancer: its relationship to estradiol and epidermal growth factor receptors and to tumor-node-metastasis staging. , 1992, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[22]  M. Dowsett,et al.  Aromatase inhibitors: basic and clinical studies. , 1987, Journal of steroid biochemistry.

[23]  S. Ebbs,et al.  Trial of aminoglutethimide vs hydrocortisone as second-line hormone treatment of advanced breast cancer. , 1993, European journal of surgical oncology : the journal of the European Society of Surgical Oncology and the British Association of Surgical Oncology.

[24]  N. Ibrahim,et al.  Aromatase Inhibitors: Current Status , 1995, American journal of clinical oncology.

[25]  P. Queirolo,et al.  Second‐Line Hormonotherapy for Breast Cancer: Uselessness of First‐Line Continuation , 1993, American journal of clinical oncology.

[26]  P. Dombernowsky,et al.  Letrozole, a new oral aromatase inhibitor for advanced breast cancer: double-blind randomized trial showing a dose effect and improved efficacy and tolerability compared with megestrol acetate. , 1998, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[27]  C. Bowden,et al.  Pharmacology of vorozole , 1993, The Journal of Steroid Biochemistry and Molecular Biology.

[28]  G. Evans,et al.  Weight changes in women with metastatic breast cancer treated with megestrol acetate: a comparison of standard versus high-dose therapy. , 1990, Seminars in oncology.

[29]  J. Thijssen,et al.  Inhibition of breast cancer tissue aromatase activity and estrogen concentrations by the third-generation aromatase inhibitor vorozole. , 1997, Cancer research.

[30]  M. Dowsett,et al.  Aromatase inhibitors in human breast cancer , 1989 .

[31]  R. D. Hunter,et al.  WHO Handbook for Reporting Results of Cancer Treatment , 1980 .

[32]  R. Gelber,et al.  Endocrine therapies of breast cancer. , 1996, Seminars in oncology.

[33]  N. Mantel Evaluation of survival data and two new rank order statistics arising in its consideration. , 1966, Cancer chemotherapy reports.

[34]  C. Spurr,et al.  High- versus standard-dose megestrol acetate in women with advanced breast cancer: a phase III trial of the Piedmont Oncology Association. , 1990, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[35]  M. Dowsett,et al.  4-hydroxyandrostenedione: a new treatment for postmenopausal patients with breast cancer. , 1992, European journal of cancer.