Single and Multiple Dose Pharmacokinetic Evaluation of Flutamide in Normal Geriatric Volunteers

Overview

Journal J Clin Pharmacol

Publisher Wiley

Specialty Pharmacology

Date 1989 Jun 1

PMID 2754024

Citations 16

Authors

E. Radwanski

G Perentesis

S SYMCHOWICZ

N Zampaglione

Affiliations

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Abstract

Single dose and steady-state pharmacokinetics of flutamide (F) and its active plasma metabolite, hydroxyflutamide (HF) were studied in twelve healthy geriatric volunteers administered 250 mg flutamide capsules on day 1 and 250 mg flutamide capsules three times a day on days 2 through 9. After oral administration, F was rapidly absorbed and metabolized. It was present in the plasma in small and variable concentrations, which precluded quantitative assessment of pharmacokinetic parameters for individual subjects. Steady-state plasma concentrations were reached on or before Day 6. The mean steady state Cmax (Day 9), 112.7 ng/ml, occurred at 1.3 hr. Pharmacokinetic analysis of mean data at steady-state gave a distribution and elimination half-life of 0.8 hr and 7.8 hours, respectively. The plasma levels for HF were much higher and less variable than F. The mean Cmax for HF averaged 894 ng/ml at 2.7 hours after a single dose and 1719 ng/ml (Day 9) at 1.9 hr after multiple doses. The distribution and elimination half-lives of HF at steady-state were 1.9 and 9.6 hours, respectively. The steady-state HF plasma concentrations were also achieved on or before Day 6 and were approximately twice those obtained after a single dose. From this study, it has been demonstrated that the pharmacokinetics of F and HF do not change appreciably upon multiple dosing of 250 mg F capsule given three times a day.

Citing Articles

Next Generation Risk Assessment of the Anti-Androgen Flutamide Including the Contribution of Its Active Metabolite Hydroxyflutamide.

van Tongeren T, Carmichael P, Rietjens I, Li H Front Toxicol. 2022; 4:881235.

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Employing Dietary Comparators to Perform Risk Assessments for Anti-Androgens Without Using Animal Data.

Dent M, Li H, Carmichael P, Martin F Toxicol Sci. 2018; 167(2):375-384.

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Enzalutamide and blocking androgen receptor in advanced prostate cancer: lessons learnt from the history of drug development of antiandrogens.

Ito Y, Sadar M Res Rep Urol. 2018; 10:23-32.

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Investigation of the In Vitro and In Vivo efficiency of RM-532-105, a 17β-hydroxysteroid dehydrogenase type 3 inhibitor, in LAPC-4 prostate cancer cell and tumor models.

Kenmogne L, Roy J, Maltais R, Rouleau M, Neveu B, Pouliot F PLoS One. 2017; 12(2):e0171871.

PMID: 28182747 PMC: 5300232. DOI: 10.1371/journal.pone.0171871.

Identification of the Additional Mitochondrial Liabilities of 2-Hydroxyflutamide When Compared With its Parent Compound, Flutamide in HepG2 Cells.

Ball A, Kamalian L, Alfirevic A, Lyon J, Chadwick A Toxicol Sci. 2016; 153(2):341-51.

PMID: 27413113 PMC: 5036617. DOI: 10.1093/toxsci/kfw126.