Fluoxetine, a selective serotonin uptake inhibitor

Fluoxetine is a selective serotonin uptake inhibitor in man. Platelets harvested from subjects to whom fluoxetine was administered (30 mg daily for 1 wk) had a diminished ability to accumulate 3 H‐serotonin. The inhibition of uptake was positively correlated with the plasma concentrations of fluoxetine. Plasma from fluoxetine‐treated subjects also inhibited the uptake of 3 H‐serotonin by platelets obtained from nontreated subjects. Fluoxetine was without effect on the noradrenergic nerve endings; pressor effects induced after the administration of norepinephrine or tyramine were similar whether subjects were receiving fluoxetine or placebo. Fluoxetine administration for 30 days produced similar pharmacologic effects as after the 7‐day study and included: (1) no change in sensitivity to the pressor effects of tyramine and norepinephrine and (2) marked inhibition in the uptake of 3H‐serotonin by platelets harvested from subjects on this regimen. In addition, fluoxetine caused a diminution of the concentration of endogenous serotonin in platelets, resulting in serotonin levels of only 20% of control. Fluoxetine was well absorbed and achieved peak plasma concentration at 6 hr after administration. Fluoxetine and the major metabolite, norfluoxetine, appeared to reach a steady state within 12 to 14 days. Fluoxetine, administered in single doses of 1 to 90 mg produced no behavioral or adverse effects. Similarly, after 1 wk of fluoxetine administration, no behavioral or adverse effects were observed.