ABCA1 Mediates Unfolding of Apolipoprotein AI N Terminus on the Cell Surface Before Lipidation and Release of Nascent High-Density Lipoprotein

Author:

Wang Shuhui1,Gulshan Kailash1,Brubaker Gregory1,Hazen Stanley L.1,Smith Jonathan D.1

Affiliation:

1. From the Department of Cellular and Molecular Medicine (S.W., K.S., G.B., S.L.H., J.D.S.), and Department of Cardiovascular Medicine (S.L.H., J.D.S.), Cleveland Clinic, Cleveland OH; and Department of Cardiology, the Second Xiangya Hospital of Central South University, Changsha, Hunan, PR China (S.W.).

Abstract

Objective— To gain insight into the mechanism by which ABCA1 generates nascent high-density lipoprotein. Approach and Results— HEK293 cells were stably transfected with ABCA1 vectors, encoding wild type, and the W590S and C1477R Tangier disease mutation isoforms, along with the K939M ATP-binding domain mutant. Apolipoprotein AI (ApoAI) binding, plasma membrane remodeling, cholesterol efflux, apoAI cell surface unfolding, and apoAI cell surface lipidation were determined, the latter 2 measured using novel fluorescent apoAI indicators. The W590S isoform had decreased plasma membrane remodeling and lipid efflux activities, and the C1477R isoform had decreased apoAI binding, and lipid efflux activities, whereas the K939M isoform did not bind apoAI, remodel the membrane, or efflux cholesterol. However, all ABCA1 isoforms led to apoAI unfolding at the cell surface, which was higher for the isoforms that increased apoAI binding. ApoAI lipidation was not detected on ABCA1-expressing cells, only in the conditioned medium, consistent with rapid release of nascent high-density lipoprotein from ABCA1-expressing cells. Conclusions— We identified a third activity of ABCA1, the ability to unfold the N terminus of apoAI on the cell surface. Our results support a model in which unfolded apoAI on the cell surface is an intermediate in its lipidation and that, once apoAI is lipidated, it forms an unstable structure that is rapidly released from the cells to generate high-density lipoprotein.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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