Your search keyword '"Ueda, Masataka"' showing total 2 results

1. Flutamide-induced hepatic dysfunction in relation to steady-state plasma concentrations of flutamide and its metabolites.

Author

Aizawa Y, Ikemoto I, Kishimoto K, Wada T, Yamazaki H, Ohishi Y, Kiyota H, Furuta N, Suzuki H, and Ueda M

Subjects

Aged, Aged, 80 and over, Androgen Antagonists therapeutic use, Flutamide therapeutic use, Humans, Liver physiopathology, Male, Middle Aged, Prospective Studies, Prostatic Neoplasms blood, Prostatic Neoplasms drug therapy, Prostatic Neoplasms physiopathology, Androgen Antagonists adverse effects, Androgen Antagonists blood, Flutamide adverse effects, Flutamide blood, Liver drug effects

Abstract

The frequency, severity, and outcome of flutamide-induced hepatic injury were prospectively evaluated in 55 patients with prostate cancer who received 125 mg of flutamide 3 times a day (daily dose: 375 mg) combined with an agonistic analogue of luteinizing hormone-releasing hormone. In addition, we examined plasma and urine concentrations of flutamide and its major metabolites 4 weeks after the beginning of flutamide therapy, and evaluated their significance in predicting flutamide-induced hepatic dysfunction. Hepatic function could be assessed in 50 patients and hepatic dysfunction during therapy was observed in 9 patients (18%); 3 patients (6%) were classified as having moderate liver dysfunction and 6 (12%) were classified as having mild liver dysfunction. The steady-state plasma levels of flutamide and its biologic active metabolite, hydroxyflutamide (OH-Flu), were not related to hepatic dysfunction. However, the concentration of another major metabolite, 4-nitro-3-(trifluoromethyl)phenylamine (FLU-1) was considerably higher in 2 patients who developed clinically significant hepatic dysfunction. These findings suggest that clinically significant hepatic dysfunction could be induced in patients with compromised flutamide metabolism, which leads to a high concentration of FLU-1. Based on results of this study, we propose that plasma FLU-1 levels are one of the predictive factors for flutamide-induced hepatic dysfunction. This hypothesis will be confirmed in a large-scale study.

Published

2003

2. Risk factor of liver disorders caused by flutamide--statistical analysis using multivariate logistic regression analysis

Author

WADA, Tetsuro, UEDA, Masataka, ABE, Kazuhiro, KOBARI, Toshihiko, YAMAZAKI, Haruki, NAKATA, Joujirou, IKEMOTO, Isao, OHISHI, Yukihiko, and AIZAWA, Yosio

Subjects

Prostate cancer, Liver disorder, 494.9, Adverse effect, Flutamide

Abstract

肝障害の発生率は33/123で, 64%の症例は9ヵ月以内に発症していた.独立項目のχ二乗検定によるとBMI, 肝障害の既往, GPTの高値の3項目が肝障害の発生に有意と判定された.SASによる多変量解析による検討では, 肝障害の既往とGPTの高値が肝障害を増加させ, 喫煙経験が肝障害を低下させる, The antiandrogenic drug, flutamide (Odyne), is widely used in the treatment of carcinoma of prostate. It is well known that flutamide has adverse effects of liver disorders. To ascertain the risk of liver disorders before administering this drug, past history and lifestyle preferences were resurveyed in 123 patients who had been treated with flutamide. The results obtained were assessed in relation to the occurrence of liver disorders by multivariate logistic regression analysis. The incidence of liver disorders was 26% (33/123), with 64% of the disorders occurring within 9 months. The chi-square test for dependent variables revealed that three variables, i.e., body mass index, past history of liver disorders and elevated glutamic-pyruvic transaminase levels were significantly related to the incidence of liver disorders (p > 0.05). Multivariate analysis indicated that a history of liver disorders and elevated alanine aminotransferase (ALT) levels were related to a higher incidence of liver disorders. Elevated ALT levels were associated with a higher incidence of liver disorders and smoking was related to a lower incidence of the liver disorders.

Published

1999