ABCA1 overexpression leads to hyperalphalipoproteinemia and increased biliary cholesterol excretion in transgenic mice
Boris L. Vaisman, … , H. Bryan Brewer Jr., Silvia Santamarina-Fojo
Boris L. Vaisman, … , H. Bryan Brewer Jr., Silvia Santamarina-Fojo
Published July 15, 2001
Citation Information: J Clin Invest. 2001;108(2):303-309. https://doi.org/10.1172/JCI12517.
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Article

ABCA1 overexpression leads to hyperalphalipoproteinemia and increased biliary cholesterol excretion in transgenic mice

Abstract

The discovery of the ABCA1 lipid transporter has generated interest in modulating human plasma HDL levels and atherogenic risk by enhancing ABCA1 gene expression. To determine if increased ABCA1 expression modulates HDL metabolism in vivo, we generated transgenic mice that overexpress human ABCA1 (hABCA1-Tg). Hepatic and macrophage expression of hABCA1 enhanced macrophage cholesterol efflux to apoA-I; increased plasma cholesterol, cholesteryl esters (CEs), free cholesterol, phospholipids, HDL cholesterol, and apoA-I and apoB levels; and led to the accumulation of apoE-rich HDL1. ABCA1 transgene expression delayed 125I-apoA-I catabolism in both liver and kidney, leading to increased plasma apoA-I levels, but had no effect on apoB secretion after infusion of Triton WR1339. Although the plasma clearance of HDL-CE was not significantly altered in hABCA1-Tg mice, the net hepatic delivery of exogenous 3H-CEt-HDL, which is dependent on the HDL pool size, was increased 1.5-fold. In addition, the cholesterol and phospholipid concentrations in hABCA1-Tg bile were increased 1.8-fold. These studies show that steady-state overexpression of ABCA1 in vivo (a) raises plasma apoB levels without altering apoB secretion and (b) raises plasma HDL-C and apoA-I levels, facilitating hepatic reverse cholesterol transport and biliary cholesterol excretion. Similar metabolic changes may modify atherogenic risk in humans.

Authors

Boris L. Vaisman, Gilles Lambert, Marcelo Amar, Charles Joyce, Toshimitsu Ito, Robert D. Shamburek, William J. Cain, Jamila Fruchart-Najib, Edward D. Neufeld, Alan T. Remaley, H. Bryan Brewer Jr., Silvia Santamarina-Fojo

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VLDL-apoB production after Triton WR1399 infusion. Control (n = 5) and h...
VLDL-apoB production after Triton WR1399 infusion. Control (n = 5) and hABCA1-A Tg (n = 5) mice were injected with Triton WR1399 to block lipolysis and 35S-methionine to label newly synthesized proteins. The mice were bled 3 hours after Triton infusion and VLDL isolated by ultracentrifugation (d = 1.006) was analyzed by either immunoblotting with anti-apoB antibodies or quantification of 35S-methionine incorporation into apoB-100 and apoB-48 (see below). The mean apoB value for control mice (n = 5) was calculated. The value of hABCA1-A Tg mice (n = 5) expressed as a percentage relative to the mean apoB value for control mice was: for apoB-100, 95 ± 11%, and for apoB-48, 103 ± 7% (P > 0.05). STD, standard.