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Structure and transport mechanism of the human cholesterol transporter ABCG1

Published:25 January 2022 DOI: 10.1016/j.celrep.2022.110298 PMID: 35081353
Da Xu, Yanyan Li, Fengrui Yang, Cai-Rong Sun, Jinheng Pan, Liang Wang, Zhi-Peng Chen, Shu-Cheng Fang, Xuebiao Yao, Wen-Tao Hou, Cong-Zhao Zhou, Yuxing Chen

Abstract

The reverse cholesterol transport pathway is responsible for the maintenance of human cholesterol homeostasis, an imbalance of which usually leads to atherosclerosis. As a key component of this pathway, the ATP-binding cassette transporter ABCG1 forwards cellular cholesterol to the extracellular acceptor nascent high-density lipoprotein (HDL). Here, we report a 3.26-? cryo-electron microscopy structure of cholesterol-bound ABCG1 in an inward-facing conformation, which represents a turnover condition upon ATP binding. Structural analyses combined with functional assays reveals that a cluster of conserved hydrophobic residues, in addition to two sphingomyelins, constitute a well-defined cholesterol-binding cavity. The exit of this cavity is closed by three pairs of conserved Phe residues, which constitute a hydrophobic path for the release of cholesterol in an acceptor concentration-dependent manner. Overall, we propose an ABCG1-driven cholesterol transport cycle initiated by sphingomyelin-assisted cholesterol recruitment and accomplished by the release of cholesterol to HDL.

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