Objective: To study the influence of the lipase inhibitor orlistat on the pharmacokinetics of the antihypertensive drugs atenolol,
furosemide, captopril and nifedipine.
Four open-label, crossover studies were performed on six to eight healthy male volunteers. Orlistat was given in doses of
50 mg 3 times daily mid-meal for 7 (nifedipine and captopril) or 8 days (atenolol and furosemide). The four antihypertensive
drugs (atenolol 100-mg tablet, furosemide 40-mg tablet, captopril 50-mg tablet and nifedipine 20-mg slow-release tablet) were
administered in single doses twice, once before and once together, with orlistat at the end of the orlistat treatment period.
The plasma concentration time profiles and the pharmacokinetic parameters estimated for these drugs were in the expected range,
except for furosemide, whose bioavailability was lower than reported in the literature. This was probably due to the fact
that furosemide was given during a meal. There were minor, but statistically significant, differences in one of the pharmacokinetic
parameters of furosemide and nifedipine (no difference for captopril and atenolol) when these drugs were given alone and in
combination with orlistat: the half-life of furosemide was slightly longer, the time to peak plasma concentrations of nifedipine
was slightly longer. None of these are considered to be clinically significant changes.
The lipase inhibitor orlistat given 50 mg 3 times daily does not alter the pharmacokinetics of atenolol, furosemide, nifedipine
and captopril to a clinically significant extent.
Key words Orlistat - Furosemide - Atenolol - Captopril - Nifedipine; pharmacokinetics - healthy volunteers
Received: 15 November 1995/Accepted in revised form: 22 February 1996