Abstract

Niflumic acid (NFA) is a member of the fenamate class of nonsteroidal anti-inflammatory drugs. This compound and its derivatives are used worldwide clinically for the relief of chronic and acute pain. NFA is also a commonly used blocker of voltage-gated chloride channels. Here we present evidence that NFA is an efficient blocker of chloride-permeable glycine receptors (GlyRs) with subunit heterogeneity of action. Using the whole-cell configuration of patch-clamp recordings and molecular modeling, we analyzed the action of NFA on homomeric α1ΔIns, α2B, α3L, and heteromeric α1β and α2β GlyRs expressed in CHO cells. NFA inhibited glycine-induced currents in a voltage-dependent manner and its blocking potency in α2 and α3 GlyRs was higher than that in α1 GlyR. The Woodhull analysis suggests that NFA blocks α1 and α2 GlyRs at the fractional electrical distances of 0.16 and 0.65 from the external membrane surface, respectively. Thus, NFA binding site in α1 GlyR is closer to the external part of the membrane, while in α2 GlyR it is significantly deeper in the pore. Mutation G254A at the cytoplasmic part of the α1 GlyR pore-lining TM2 helix (level 2′) increased the NFA blocking potency, while incorporation of the β subunit did not have a significant effect. The Hill plot analysis suggests that α1 and α2 GlyRs are preferably blocked by two and one NFA molecules, respectively. Molecular modeling using Monte Carlo energy minimizations provides the structural rationale for the experimental data and proposes more than one interaction site along the pore where NFA can suppress the ion permeation.

Highlights

  • The main inhibitory drive in mammalian central nervous system (CNS) is provided by chloride (Cl−)-permeable GABAAand glycine receptors (GlyRs) (Sigel and Steinmann, 2012; Lynagh and Pless, 2014)

  • We found that the apparent Niflumic acid (NFA) affinity, the voltage-dependence and the depth of its binding in the membrane strongly depend on the GlyR subunit composition, which possess different TM2 transmembrane helices

  • The NFA ability to modulate currents in different GlyR subtypes was determined using a whole-cell configuration of patch-clamp technique

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Summary

Introduction

The main inhibitory drive in mammalian CNS is provided by chloride (Cl−)-permeable GABAAand glycine receptors (GlyRs) (Sigel and Steinmann, 2012; Lynagh and Pless, 2014). GlyRs participate in the movement control, perception of visual, acoustic and sensory signals and pain sensation (Harvey et al, 2004; Betz and Laube, 2006). Dysfunction of these receptors is associated with hyperekplexia and temporal lobe seizures accompanied by memory deficits (Lynch, 2009; Schaefer et al, 2012; Zuliani et al, 2014). These subunits assemble to form homopentameric α GlyRs and heteropentameric α/β GlyRs (Lynch, 2004)

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