Literature DB >> 1756260

A phase I/II study of high-dose megestrol acetate in the treatment of metastatic breast cancer.

H L Parnes1, J S Abrams, N S Tchekmedyian, N Tait, J Aisner.   

Abstract

A dose-response relationship has been suggested for medroxyprogesterone acetate in the treatment of advanced breast cancer. To determine the tolerability and efficacy of increasing doses of megestrol acetate in the treatment of metastatic breast cancer, we conducted a phase I/II study among 57 patients. Three patients each received 480, 800, and 1280 mg/d; 48 patients received 1600 mg/d. Of the 57 patients, 56 patients had had disease progression on prior hormone therapy, chemotherapy, or both. Twenty-seven patients had previously received standard-dose MA (160 mg/d). Among the 37 patients with measurable disease, high-dose megestrol acetate (HDMA) produced 6 (16%) complete responses (CRs) and 6 (16%) partial responses (PRs); 11 patients achieved stable disease (SD). HDMA resulted in improvement or stabilization in 12 of the 20 patients with evaluable, non-measurable disease. There were no responses among the 6 patients with liver metastases. Among the 27 patients who were previously treated with standard-dose MA, including 9 patients with primary treatment failure, HDMA resulted in 1 CR, 3 PRs, and 10 SD. Toxicities, which were mild and reversible, included fluid retention, hypertension, hyperglycemia, and mild congestive heart failure. Two patients had superficial phlebitis. The most profound side effect was weight gain which occurred in 43 patients (75%). This study suggests a dose-response relationship for MA in the treatment of advanced breast cancer. A randomized trial to determine the optimal dose is ongoing.

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Year:  1991        PMID: 1756260     DOI: 10.1007/bf01990033

Source DB:  PubMed          Journal:  Breast Cancer Res Treat        ISSN: 0167-6806            Impact factor:   4.872


  29 in total

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Review 2.  Quantitation of tumor response to anti-neoplastic therapy.

Authors:  S A Grossman; P A Burch
Journal:  Semin Oncol       Date:  1988-10       Impact factor: 4.929

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Authors:  J H von Roenn; R L Murphy; K M Weber; L M Williams; S A Weitzman
Journal:  Ann Intern Med       Date:  1988-11-15       Impact factor: 25.391

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Authors:  L R Morgan
Journal:  Semin Oncol       Date:  1985-03       Impact factor: 4.929

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Journal:  Semin Oncol       Date:  1985-03       Impact factor: 4.929

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Journal:  Semin Oncol       Date:  1985-03       Impact factor: 4.929

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Journal:  Semin Oncol       Date:  1985-12       Impact factor: 4.929

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Authors:  G N Hortobagyi; A U Buzdar; D Frye; H Y Yap; V Hug; K Pinnamaneni; G Fraschini; H C Halvorson; G R Blumenschein
Journal:  Breast Cancer Res Treat       Date:  1985       Impact factor: 4.872

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Journal:  Semin Oncol       Date:  1985-03       Impact factor: 4.929

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Journal:  Tumori       Date:  1978-04-30
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  3 in total

1.  Reversal of the human and murine multidrug-resistance phenotype with megestrol acetate.

Authors:  L Wang; C P Yang; S B Horwitz; P A Trail; A M Casazza
Journal:  Cancer Chemother Pharmacol       Date:  1994       Impact factor: 3.333

Review 2.  Protein calorie malnutrition and cancer therapy.

Authors:  H L Parnes; J Aisner
Journal:  Drug Saf       Date:  1992 Nov-Dec       Impact factor: 5.606

3.  A pilot study of megestrol acetate and ibuprofen in the treatment of cachexia in gastrointestinal cancer patients.

Authors:  D C McMillan; P O'Gorman; K C Fearon; C S McArdle
Journal:  Br J Cancer       Date:  1997       Impact factor: 7.640

  3 in total

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