Side-Dependent Inhibition of a Prokaryotic ClC by DIDS

Side-Dependent Inhibition of a Prokaryotic ClC by DIDS

The x-ray structure of the Escherichia coli chloride/proton antiporter ClC-ec1 provides a structural paradigm for the widespread and diverse ClC family of chloride channels and transporters. To maximize the usefulness of this paradigm, it is important to directly relate structure to function via stu...

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Bibliographic Details
Published in:Biophysical journal Vol. 89; no. 3; pp. 1721 - 1730
Main Authors: Matulef, Kimberly, Maduke, Merritt
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-09-2005
Biophysical Society
Subjects:
4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid - pharmacology
Binding Sites
Biological Transport
Channels, Receptors, and Electrical Signaling
Chloride Channels - chemistry
Chloride Channels - drug effects
Chloride Channels - physiology
Chlorides - chemistry
Crystallography, X-Ray
Cysteine - chemistry
Escherichia coli - metabolism
Escherichia coli Proteins - chemistry
Hydrogen-Ion Concentration
Ion Channel Gating
Lipid Bilayers - metabolism
Membrane Transport Proteins - chemistry
Models, Biological
Models, Molecular
Protons
Time Factors
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Summary:The x-ray structure of the Escherichia coli chloride/proton antiporter ClC-ec1 provides a structural paradigm for the widespread and diverse ClC family of chloride channels and transporters. To maximize the usefulness of this paradigm, it is important to directly relate structure to function via studies of ClC-ec1 itself; however, few functional studies of this protein have been performed. In an endeavor to develop new tools for functional analysis of ClC-ec1, we have discovered that this transporter is inhibited by the stilbenedisulfonate 4,4-diisothiocyanatostilbene-2,2′-disulfonic acid (DIDS). In planar lipid bilayers, DIDS inhibits ClC-ec1 activity reversibly, with an apparent affinity in the micromolar range. Since ClC-ec1 is randomly oriented in the bilayers, ascertaining whether DIDS inhibits from the intracellular or extracellular side required an indirect approach. Using the ClC-ec1 structure as a guide, we designed a strategy in which modification of Y445C was monitored in conjunction with inhibition by DIDS. We found that DIDS inhibits transporters specifically from the intracellular side. Transporters with their extracellular side exposed to DIDS function normally, maintaining stoichiometric proton/chloride antiport over a wide range of proton and chloride concentrations. The side-dependent nature of DIDS inhibition will be useful for generating “functionally oriented” preparations of ClC-ec1, in which DIDS is used to silence transporters in one orientation but not the other.
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Address reprint requests to Merritt Maduke, Dept. of Molecular and Cellular Physiology, B155 Beckman Center, 279 Campus Drive, Stanford, CA 94305. Tel.: 650-723-9075; Fax: 650-725-8021; E-mail: maduke@stanford.edu.
ISSN:0006-3495
1542-0086
DOI:10.1529/biophysj.105.066522