THE INFLUENCE OF CGS-16949A ON PERIPHERAL AROMATIZATION IN BREAST-CANCER PATIENTS

被引:71
作者
LONNING, PE
JACOBS, S
JONES, A
HAYNES, B
POWLES, T
DOWSETT, M
机构
[1] ROYAL MARSDEN HOSP, DEPT MED, LONDON, ENGLAND
[2] ROYAL MARSDEN HOSP, ACAD DEPT BIOCHEM, LONDON, ENGLAND
[3] ROYAL MARSDEN HOSP, ACAD DEPT BIOCHEM, SUTTON, SURREY, ENGLAND
[4] ROYAL MARSDEN HOSP, DEPT MED, SUTTON, SURREY, ENGLAND
[5] INST CANC RES, CANC RES CAMPAIGN LABS, DRUG DEV SECT, SUTTON SM2 5PX, SURREY, ENGLAND
关键词
D O I
10.1038/bjc.1991.175
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The influence of a new aromatase inhibitor, CGS 16949A on peripheral aromatisation of androstenedione into oestrone was investigated in postmenopausal women with breast cancer. A mixture of H-3 androstenedione and C-14 oestrone was injected, and all urine was collected for the following 96 h. The isotope ratio was determined in the urinary oestrogen metabolites after isolation by HPLC. Eight patients were investigated before and during treatment with CGS 16949A. At a dose of 1 mg b.d. (eight patients) CGS 16949A inhibited aromatisation by a mean value of 82.4% (range 71.3 to 93.7%). When the drug dose was escalated to 2 mg b.d. (three patients) aromatisation was inhibited by a mean of 92.6% (range 90.6 to 95.8%). These results suggest that CGS 16949A at a dose of 1 mg b.d. causes submaximal aromatase inhibition in many patients, while a dose of 2 mg b.d. seems to result in greater than 90% aromatase inhibition. These data are consistent with previous observations that the higher dose is more effective in suppression of plasma oestradiol levels.
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收藏
页码:789 / 793
页数:5
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