Structural insights into human ABCD3-mediated peroxisomal acyl-CoA translocation

Author:

Li Yang,Chen Zhi-Peng,Xu Da,Wang Liang,Cheng Meng-Ting,Zhou Cong-ZhaoORCID,Chen YuxingORCID,Hou Wen-TaoORCID

Abstract

AbstractHuman ABC transporters ABCD1–3 are all localized on the peroxisomal membrane and participate in the β-oxidation of fatty acyl-CoAs, but they differ from each other in substrate specificity. The transport of branched-chain fatty acids from cytosol to peroxisome is specifically driven by ABCD3, dysfunction of which causes severe liver diseases such as hepatosplenomegaly. Here we report two cryogenic electron microscopy (cryo-EM) structures of ABCD3 bound to phytanoyl-CoA and ATP at resolutions of 2.9 Å and 3.2 Å, respectively. A pair of phytanoyl-CoA molecules were observed in ABCD3, each binding to one transmembrane domain (TMD), which is distinct from our previously reported structure of ABCD1, where each fatty acyl-CoA molecule strongly crosslinks two TMDs. Upon ATP binding, ABCD3 exhibits a conformation that is open towards the peroxisomal matrix, leaving two extra densities corresponding to two CoA molecules deeply embedded in the translocation cavity. Structural analysis combined with substrate-stimulated ATPase activity assays indicated that the present structures might represent two states of ABCD3 in the transport cycle. These findings advance our understanding of fatty acid oxidation and the molecular pathology of related diseases.

Funder

University of Science and Technology of China

National Natural Science Foundation of China

Ministry of Science and Technology of the People's Republic of China

Publisher

Springer Science and Business Media LLC

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