5 mg testosterone complexed MK5108 research buy with hydroxypropyl-β cyclodextrin. All 13 subjects received the investigational drug formulation in random order. Wash-out between treatments was at least 7 days. Subjects had serial blood samples drawn via an intravenous catheter. Pharmacokinetic parameters were monitored at baseline (−10 min) and (at 5, 10, 15, 20, 25, 30, 60, 90, 120, 135, 145, 165, 180, 195, 210, 225, 240, 270, 300, 330, 360, 390, 450, 570, 690, 810, 930, 1,590 min) after dosing. Measurement of total testosterone, free testosterone, and dihydrotestosterone were performed at −10, 5,
10, 15, 20, 25, 30, 60, 90, 120, 145, 180, 240 and 1,590 minutes after dosing; buspirone and metabolite 1-(2-pyrimidinyl)-piperazine at −10, 10, 30, 60, 90, 120, 135, 145, 165, 180, 195, 210, 225, 240, 270, 300, 330, 360, 390, 450, 570, 690, 810, 930, 1,590 minutes after dosing. For each admission period,
subjects were instructed to come to the study site on the evening prior to dose administration where vital signs were checked (including ECG) and urine drug test, pregnancy test, and alcohol breath analysis were performed. During the admission period, the subjects received low calorie meals on site and decaffeinated coffee and tea to minimize the influence on pharmacokinetic parameters. Drug, alcohol, and pregnancy tests were performed prior to experimental sessions. 2.3 Medication and Dosing The combination tablet is a menthol-flavored white tablet of 9 mm in diameter for sublingual administration Givinostat molecular weight followed by oral administration. The quickly dissolving outer coating, applied by film coating the tablet, delivers cyclodextrin-complexed testosterone (0.5 mg) sublingually, click here and the time-delayed-release core delivers buspirone (10 mg) 2.5 hours later. The outer coating comprises testosterone, excipients, and a menthol flavor to guide the disappearance of the coating. The testosterone coating is designed to fully dissolve and Suplatast tosilate to obtain a fast and complete absorption via the mucosal membranes under the tongue. The time-delayed-release core containing the buspirone has been designed
on the basis of in-vitro release studies of US Pharmacopeia (USP) II and III, to release the buspirone in a pulsatile manner, approximately 2.5 hours after oral administration. This method of release is accomplished through the use of a polymer coating of ethylcellulose which allows for a slow permeation of water in a pH-independent manner. At the predetermined time, the polymer coating ruptures at the edge of the tablet. The complete disintegrated core of the inner tablet is released immediately, after which there is no delay for the dissolution of the buspirone in the surrounding fluid. The two formulations were administered by a trained research associate and controlled by a second research associate. For the testosterone component of F1, a 1 mg/mL testosterone cyclodextrin complex solution was used; the solution was administered with a micropipette (e.g.