Abstract 227: Measuring HDL-apolipoprotein A-I Exchange By Subclass In Reconstituted And Human HDL

Abstract

Objective: Levels of high density lipoprotein (HDL) are inversely associated with cardiovascular disease risk. HDL particles contain a diverse array of lipids, cholesterol, and proteins, and exist over a range of sizes ranging from about 8 nm to about 17 nm diameter, but it is not well understood how HDL size affects its function. In this study we examine the effect of HDL particle size on the rate of HDL-apolipoprotein A-I (apoA-I) exchange in reconstituted and human HDL particles. Method and Results: Reconstituted HDL particles were synthesized from 16:0-18:1n-9 PC, cholesterol, and recombinant apoA-I. Human HDL was isolated from plasma from healthy volunteers by density gradient ultracentrifugation. In both cases, the HDL was further separated by subclass using size exclusion chromatography. ApoA-I exchange was measured by incubating fluorescently-labeled, lipid-free apoA-I with HDL and quantifying the fluorescent signal appearing in the HDL region versus the lipid-free region of a nondenaturing gel over time. ApoA-I exchange rates increased inversely with particle size in both reconstituted and human HDL, with medium-sized HDL particles exhibiting twofold faster exchange rates compared to the largest HDL particles. Conclusions: Smaller HDL particles exhibit faster rates of HDL-apoA-I exchange in both reconstituted and human HDL particles. Reconstituted HDL particles provide an accurate approximation of apoA-I exchange in human HDL particles.