External amino acid residues of insect GABA receptor channels dictate the action of the isoxazoline ectoparasiticide fluralaner

Author:

Asahi Miho1,Yamato Kohei2,Ozoe Fumiyo23,Ozoe Yoshihisa23ORCID

Affiliation:

1. Biological Research Laboratories Nissan Chemical Corporation Shiraoka Saitama Japan

2. Faculty of Life and Environmental Sciences Shimane University Matsue Shimane Japan

3. Interdisciplinary Institute for Science Research, Organization for Research and Academic Information Shimane University Matsue Shimane Japan

Abstract

AbstractBACKGROUNDFluralaner is the first isoxazoline ectoparasiticide developed to protect companion animals from fleas and ticks. Fluralaner primarily inhibits arthropod γ‐aminobutyric acid receptors (GABARs), which are ligand‐gated ion channels comprising five subunits arranged around the channel pore. We previously reported that the action site of fluralaner resides at the M1–M3 transmembrane interface between adjacent GABAR subunits. To investigate whether fluralaner interacts with the second transmembrane segment (M2) located deep in the interface, we generated four housefly RDL GABAR mutants with non‐conservative amino acid substitutions in the M2 region.RESULTSElectrophysiological analysis of GABARs expressed in Xenopus oocytes indicated that S313A and S314A mutants exhibited fluralaner sensitivities similar to that of the wild type. M312S mutant exhibited approximately seven‐fold lower sensitivity than that of the wild type. Notably, the N316L mutant was almost insensitive to fluralaner.CONCLUSIONThe findings of this study indicate that the conserved external amino acid residues of insect GABAR channels play a critical role in the antagonistic effect of fluralaner. © 2023 Society of Chemical Industry.

Publisher

Wiley

Subject

Insect Science,Agronomy and Crop Science,General Medicine

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