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W546 stacking disruption traps the human porphyrin transporter ABCB6 in an outward-facing transient state

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Abstract
Human ATP-binding cassette transporter subfamily B6 (ABCB6) is a mitochondrial ATP-driven pump that translocates porphyrins from the cytoplasm into mitochondria for heme biosynthesis. Within the transport pathway, a conserved aromatic residue W546 located in each monomer plays a pivotal role in stabilizing the occluded conformation via pi-stacking interactions. Herein, we employed cryo-electron microscopy to investigate the structural consequences of a single W546A mutation in ABCB6, both in detergent micelles and nanodiscs. The results demonstrate that the W546A mutation alters the conformational dynamics of detergent-purified ABCB6, leading to entrapment of the transporter in an outward-facing transient state. However, in the nanodisc system, we observed a direct interaction between the transporter and a phospholipid molecule that compensates for the absence of the W546 residue, thereby facilitating the normal conformational transition of the transporter toward the occluded state following ATP hydrolysis. The findings also reveal that adoption of the outward-facing conformation causes charge repulsion between ABCB6 and the bound substrate, and rearrangement of key interacting residues at the substrate-binding site. Consequently, the affinity for the substrate is significantly reduced, facilitating its release from the transporter. W546A mutation in Human ATP-binding cassette transporter subfamily B6 (ABCB6) alters its conformational dynamics, leading to reduced substrate affinity and facilitating release from the transporter.
Author(s)
Lee, Sang SooPark, Jun GyouJang, EunhongChoi, Seung HunKim, SubinKim, Ji WonJin, Mi Sun
Issued Date
2023-09
Type
Article
DOI
10.1038/s42003-023-05339-3
URI
https://scholar.gist.ac.kr/handle/local/10020
Publisher
NATURE PORTFOLIO
Citation
COMMUNICATIONS BIOLOGY, v.6, no.1
ISSN
2399-3642
Appears in Collections:
Department of Life Sciences > 1. Journal Articles
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