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Circulation. 2002;106:1943-1948
Published online before print September 3, 2002, doi: 10.1161/01.CIR.0000034044.95911.DC
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(Circulation. 2002;106:1943.)
© 2002 American Heart Association, Inc.


Clinical Investigation and Reports

Inhibition of Intestinal Cholesterol Absorption by Ezetimibe in Humans

Thomas Sudhop, MD*; Dieter Lütjohann, PhD, MS*; Annette Kodal, MD; Michael Igel, MD; Diane L. Tribble, PhD; Sukrut Shah, PhD; Inna Perevozskaya, PhD; Klaus von Bergmann, MD

From the Department of Clinical Pharmacology (T.S., D.L., A.K., M.I., K.v.B.), University of Bonn, Germany; and Clinical Research (D.L.T., S.S., I.P.), Merck Research Laboratories, Rahway, NJ.

Correspondence to Prof Klaus von Bergmann, MD, Dept of Clinical Pharmacology, University of Bonn, Sigmund-Freud-Str. 25, 53105 Bonn/Germany. E-mail vonbergmann{at}uni-bonn.de

Background— Ezetimibe has been shown to inhibit cholesterol absorption in animal models, but studies on cholesterol absorption in humans have not been performed thus far.

Methods and Results— The effect of ezetimibe (10 mg/d) on cholesterol absorption and synthesis, sterol excretion, and plasma concentrations of cholesterol and noncholesterol sterols was investigated in a randomized, double-blind, placebo-controlled, crossover study in 18 patients with mild to moderate hypercholesterolemia. Treatment periods lasted 2 weeks with an intervening 2-week washout period. Fractional cholesterol absorption rates averaged 49.8±13.8% on placebo and 22.7±25.8% on ezetimibe, indicating a reduction of 54% (geometric mean ratio; P< 0.001). Cholesterol synthesis increased by 89% from 931±1027 mg/d on placebo to 1763±1098 mg/d on ezetimibe (P<0.001), while the ratio of lathosterol-to-cholesterol, an indirect marker of cholesterol synthesis, was increased by 72% (P<0.001). Bile acid synthesis was insignificantly increased (placebo: 264±209 mg/d, ezetimibe: 308±184 mg/d; P=0.068). Mean percent changes from baseline for LDL and total cholesterol after ezetimibe treatment were -20.4% and -15.1%, respectively (P<0.001 for both), whereas campesterol and sitosterol were decreased by -48% and - 41%, respectively.

Conclusion— In humans, ezetimibe inhibits cholesterol absorption and promotes a compensatory increase of cholesterol synthesis, followed by clinically relevant reductions in LDL and total cholesterol concentrations. Ezetimibe also reduces plasma concentrations of the noncholesterol sterols sitosterol and campesterol, suggesting an effect on the absorption of these compounds as well.


Key Words: ezetimibe • cholesterol absorption • cholesterol synthesis • lathosterol • plant sterols




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