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EFFECT OF THE ACYL-COA-CHOLESTEROL ACYLTRANSFERASE INHIBITOR DUP-128 ON CHOLESTEROL ABSORPTION AND SERUM-CHOLESTEROL IN HUMANS

Authors

HAINER JW TERRY JG CONNELL JM ZYRUK H JENKINS RM SHAND DL GILLIES PJ LIVAK KJ HUNT TL CROUSE JR

Citation

Jw. Hainer et al., EFFECT OF THE ACYL-COA-CHOLESTEROL ACYLTRANSFERASE INHIBITOR DUP-128 ON CHOLESTEROL ABSORPTION AND SERUM-CHOLESTEROL IN HUMANS, Clinical pharmacology and therapeutics, 56(1), 1994, pp. 65-74

Citations number

Categorie Soggetti

Pharmacology & Pharmacy

Journal title

Clinical pharmacology and therapeutics → ACNP

ISSN journal

00099236

Volume

Issue

Year of publication

1994

Pages

65 - 74

Database

ISI

SICI code

0009-9236(1994)56:1<65:EOTAAI>2.0.ZU;2-D

Abstract

Intestinal cholesterol esterification by the enzyme acyl-CoA: choleste rol acyltransferase (ACAT) is a presumed prerequisite for cholesterol absorption. We evaluated the effect of a potent, poorly absorbed ACAT inhibitor (DuP 128: iphenyl-1H-imidazol-2-ylthio)pentyl]-N-heptylurea) on cholesterol absorption in a randomized trial. Thirty subjects rece ived DuP 128 for 7 weeks, 10 each at 900 mg per day, 1800 mg per day, and 3600 mg per day;six subjects received placebo; and nine subjects r eceived I gm neomycin twice a day. Cholesterol absorption determinatio ns used a continuous dual isotope C-14-cholesterol and H-3-beta sitost erol method. DuP 128 (pooled doses) induced at 14.4% +/- 11.4% reducti on in cholesterol absorption (p < 0.05 versus placebo): 17.6% +/- 8.4% at 900 mg, 9.1% +/- 11.4% at 1800 mg, and 17.1% +/- 12.9% at 3600 mg. Neomycin induced a 26.4% +/- 10.7% reduction (p < 0.01). After 6 week s, neomycin reduced serum total and low-density lipoprotein cholestero l by 22.4% +/- 9.2% and 24.0% +/- 11.6%, respectively (p < 0.01 versus placebo). DuP 128 induced reductions of 3.9% +/- 11% (difference not significant) and 4.95% +/- 14.3% (p = 0.05). ACAT inhibitors limit cho lesterol absorption in humans; however, the magnitude of the effect, a s exemplified by DuP 128, is small.