Systemic bioavailability of acebutolol in man

## Introduction Recently, the pharmacokinetics of timolol, a padrenergic blocking agent and a propranolol analog, were reported for normal volunteers and uremic patients after oral administration. Clinically, timolol is more potent when compared to propranolol and alprenolol as an antihypertensive

## Abstract Fourteen normal male subjects were given either 60 mg or 180mg of terfenadine suspension in a randomized two‐way crossover study. Peak plasma concentrations of 1.544 ± 0.726 (mean ± S.D.) ng ml^−1^ were obtained in 0.786 ± 0.426 h following the 60 mg dose and displayed an AUC of 11.864

Ten healthy male volunteers received single oral doses of l00mg of medroxalol administered as a solution, a preliminary tablet formulation and a single dose of lOOmg administered intravenously in a randomized three-way crossover study. Mean terminal half-lives of 12.4, 13.4, and 11.3 h were observed

A seven-way crossover study was conducted in 14 healthy male volunteers to evaluate the relative bioavailability of seven different marketed 40 mg furosemide tablets. Each dose was administered as a single tablet after an overnight fast. and blood samples were obtained for 16 hours. Plasma was assay

In order to investigate the bioavailability and the rate-limiting step of the absorption of roquinimex, an oral solution and a tablet formulation (Linomide ® ) were given to healthy volunteers. The study was conducted as a randomized three-period crossover study in seven male and seven female health

## Abstract In this comparative bioavailability study in 12 healthy volunteers the blood level profiles and urinary recoveries of both atenolol and chlorthalidone were studied following the administration of the drug as a fixed combination (‘Tenoretic’), as a free combination, and individually, at