Abstract
AbstractCholesteryl ester transfer protein (CETP) modulates lipoprotein metabolism by transferring cholesteryl ester (CE) and triglyceride (TG) between lipoproteins. However, differences in the way CETP functions exist across species. Unlike human CETP, hamster CETP prefers TG over CE as a substrate, raising questions regarding how substrate preference may impact lipoprotein metabolism. To understand how altering the CE versus TG substrate specificity of CETP might impact lipoprotein metabolism in humans, we modified CETP expression in fat/cholesterol-fed hamsters, which have a human-like lipoprotein profile. Hamsters received adenoviruses expressing no CETP, hamster CETP, or human CETP. Total plasma CETP mass increased up to 70% in the hamster and human CETP groups. Hamsters expressing human CETP exhibited decreased endogenous hamster CETP, resulting in an overall CE:TG preference of plasma CETP that was similar to that in humans. Hamster CETP overexpression had little impact on lipoproteins, whereas human CETP expression reduced HDL by 60% without affecting LDL. HDLs were TG enriched and CE depleted and much smaller, causing the HDL3:HDL2 ratio to increase threefold. HDL from hamsters expressing human CETP supported higher LCAT activity and greater cholesterol efflux. The fecal excretion of HDL-associated CE in human CETP animals was unchanged. However, much of this cholesterol accumulated in the liver and was associated with a 1.8-fold increase in hepatic cholesterol mass. Overall, these data show in a human-like lipoprotein model that modification of CETP's lipid substrate preference selectively alters HDL concentration and function. This provides a powerful tool for modulating HDL metabolism and impacting sterol balance in vivo.
Highlights
Cholesteryl ester transfer protein (CETP) modulates lipoprotein metabolism by transferring cholesteryl ester (CE) and triglyceride (TG) between lipoproteins
Mutations of single amino acid residues in CETP are sufficient to change its preference for CE versus TG as a substrate [4], which alters the redistribution of these lipids between TG- and CE-rich lipoproteins [5]
Human and hamster CETPs have greatly different preferences for CE versus TG as a substrate. Those studies in chowfed hamsters clearly demonstrated that modification of the substrate specificity of plasma CETP drives large changes in the levels and composition of lipoproteins, especially those of HDL
Summary
Cholesteryl ester transfer protein (CETP) modulates lipoprotein metabolism by transferring cholesteryl ester (CE) and triglyceride (TG) between lipoproteins. Much of this cholesterol accumulated in the liver and was associated with a 1.8-fold increase in hepatic cholesterol mass Overall, these data show in a human-like lipoprotein model that modification of CETP's lipid substrate preference selectively alters HDL concentration and function. Human and hamster CETPs have greatly different preferences for CE versus TG as a substrate Those studies in chowfed hamsters clearly demonstrated that modification of the substrate specificity of plasma CETP drives large changes in the levels and composition of lipoproteins, especially those of HDL. Whether this preferential impact on HDL reflects the fact that HDL is the major lipoprotein in these chow-fed animals is not known.
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