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Fluoride-dependent interruption of the transport cycle of a CLC Cl-/H+ antiporter

Authors
Lim, Hyun-HoStockbridge, Randy B.Miller, Christopher
Issue Date
Nov-2013
Publisher
NATURE PUBLISHING GROUP
Citation
NATURE CHEMICAL BIOLOGY, v.9, no.11, pp.721 - +
Journal Title
NATURE CHEMICAL BIOLOGY
Volume
9
Number
11
Start Page
721
End Page
+
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/897
DOI
10.1038/NCHEMBIO.1336
ISSN
1552-4450
Abstract
Cl-/H+ antiporters of the CLC superfamily transport anions across biological membranes in varied physiological contexts. These proteins are weakly selective among anions commonly studied, including Cl-, Br-, I-, NO3- and SCN-, but they seem to be very selective against F-. The recent discovery of a new CLC clade of F-/H+ antiporters, which are highly selective for F- over Cl-, led us to investigate the mechanism of Cl--over-F- selectivity by a CLC Cl-/H+ antiporter, CLC-ec1. By subjecting purified CLC-ec1 to anion transport measurements, electrophysiological recording, equilibrium ligand-binding studies and X-ray crystallography, we show that F- binds in the Cl- transport pathway with affinity similar to Cl- but stalls the transport cycle. Examination of various mutant antiporters implies a 'lock-down' mechanism of F- inhibition, in which F-, by virtue of its unique hydrogen-bonding chemistry, greatly retards a proton-linked conformational change essential for the transport cycle of CLC-ec1.
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연구본부 (신경·혈관단위체 연구그룹)
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