Volume-activated chloride currents in HeLa cells are blocked by tamoxifen but not by a membrane impermeant quaternary analogue

Mousa Sahebgharani, Simon P. Hardy, Andrew W. Lloyd, Alan C. Hunter, Marcus C. Allen

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Background/Aims: Tamoxifen has been shown to inhibit volume activated chloride currents in many cell types. Tamoxifen has also been reported to inhibit a number of cation channels as well as cytosolic proteins such as calmodulin. The mechanism of channel block by tamoxifen is not known but three hypotheses can be proposed: i) a direct effect following binding to the channel protein from the aqueous environment or ii) a direct effect on the channel protein after partitioning into the lipid membrane or iii) an indirect mechanism via binding to intracellular regulatory proteins after diffusion across the lipid membrane. The aim of these experiments was to distinguish between these hypothoses using membrane permeant and impermeant antioestrogens. Methods: Volume activated chloride currents were recorded from single HeLa cells using whole cell patch clamp technique. The ability of tamoxifen and its membrane impermeant quaternary derivative ethylbromide tamoxifen (EBT) to inhibit these currents was examined. Results: Extracellular tamoxifen at 3μM inhibited volume activated chloride currents in HeLa cells whereas EBT had no effect up to 10μM when applied eitherto the extracellular bathing solution or the intracellular solution via the patch pipette. Conclusion: Eliminating the ability of tamoxifen to cross the plasma membrane abolishes its channel blocking activity against volume activated chloride channels in HeLa cells. Copyright © 2001 S. Karger AG, Basel.
    Original languageEnglish
    Pages (from-to)99-104
    Number of pages5
    JournalCellular Physiology and Biochemistry
    Volume11
    Issue number2
    DOIs
    Publication statusPublished - 2001

    Keywords

    • Ethyl bromide
    • Tamoxifen
    • Tamoxifen (EBT)
    • Volume activated chloride currents

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