AI Article Synopsis

  • CLC-2 is a voltage-gated chloride channel found in various mammalian tissues, particularly in the central nervous system, where its role remains unclear due to a lack of specific pharmacological tools.
  • Researchers developed AK-42, a highly selective small-molecule inhibitor of CLC-2, which shows remarkable potency and does not affect other related channels.
  • The findings indicate that AK-42 effectively inhibits CLC-2 activity in neuronal recordings, making it a valuable resource for studying the functions and effects of CLC-2 in the brain.

Article Abstract

CLC-2 is a voltage-gated chloride channel that is widely expressed in mammalian tissues. In the central nervous system, CLC-2 appears in neurons and glia. Studies to define how this channel contributes to normal and pathophysiological function in the central nervous system raise questions that remain unresolved, in part due to the absence of precise pharmacological tools for modulating CLC-2 activity. Herein, we describe the development and optimization of AK-42, a specific small-molecule inhibitor of CLC-2 with nanomolar potency (IC = 17 ± 1 nM). AK-42 displays unprecedented selectivity (>1,000-fold) over CLC-1, the closest CLC-2 homolog, and exhibits no off-target engagement against a panel of 61 common channels, receptors, and transporters expressed in brain tissue. Computational docking, validated by mutagenesis and kinetic studies, indicates that AK-42 binds to an extracellular vestibule above the channel pore. In electrophysiological recordings of mouse CA1 hippocampal pyramidal neurons, AK-42 acutely and reversibly inhibits CLC-2 currents; no effect on current is observed on brain slices taken from CLC-2 knockout mice. These results establish AK-42 as a powerful tool for investigating CLC-2 neurophysiology.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7768775PMC
http://dx.doi.org/10.1073/pnas.2009977117DOI Listing

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