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J. Biol. Chem., Vol. 265, Issue 14, 8042-8051, May, 1990
I Tabas, LL Chen, JW Clader, AT McPhail, DA Burnett, P Bartner, PR Das, BN Pramanik, MS Puar and SJ Feinmark
Acyl-coenzyme A (CoA):cholesterol acyltransferase (ACAT) catalyzes the
intracellular fatty acid esterification of cholesterol and is thought to
play a key role in lipoprotein metabolism and atherogenesis. Herein we
describe the purification and characterization of a novel pentacyclic
triterpene ester from rabbit liver that has ACAT inhibitory activity. The
inhibitor was purified by a combination of silicic acid chromatography and
preparative thin layer chromatography. The compound inhibited both rabbit
and rat liver microsomal ACAT activity with an IC50 = 20 microM. The lipid
did not inhibit fatty acid incorporation into triglycerides, diglycerides,
monoglycerides, or phospholipids nor did it inhibit plasma
lecithin:cholesterol acyltransferase activity. However, rat liver
microsomal acyl-CoA:retinol acyltransferase activity was inhibited by the
terpene ester. Kinetic data are consistent with a mechanism in which ACAT
is inhibited by the compound in an irreversible manner. The subcellular
fractionation pattern of both ACAT activity and the ACAT inhibitor were
similar in rabbit liver (both were approximately equally distributed in
membranes that pelleted at 10,000 X g and 100,000 X g). A lipid with
similar properties to the rabbit liver inhibitor was found in many other
rabbit tissues, including adrenal and spleen, as well as in human liver.
Rat liver did not contain this lipid. Structural analysis by NMR, mass
spectrometry, and x-ray crystallography indicated that the rabbit liver
inhibitor was a fatty acid ester (mostly stearate) of a pentacyclic
triterpene acid. The carbon skeleton of the triterpene moiety is a new
member of the olean-12-ene triterpene family. Both the negatively charged
carboxylic acid group of the triterpene moiety and the esterified fatty
acid group were necessary for the ACAT-inhibitory activity of the
triterpene ester. Lastly, we present preliminary data which, together with
the structural homology of the rabbit triterpene with known plant
compounds, suggest the hypothesis that the triterpene moiety of the rabbit
ACAT inhibitor arises from dietary absorption of a plant triterpene.
Rabbit and human liver contain a novel pentacyclic triterpene ester with acyl-CoA: cholesterol acyltransferase inhibitory activity
Department of Medicine, Columbia University, New York, New York 10032.
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