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Zhao C & Casida JE
Insect -aminobutyric acid receptors and isoxazoline insecticides: toxicological profiles relative to the binding sites of [3H]fluralaner, [3H]-4'-ethynyl-4-n-propylbicycloorthobenzoate, and [3H]avermectin.

J Agr Food Chem, 62(5): 1019-1024, 2014
ISSN: 0021-8561 Journal of Agricultural and Food Chemistry (PubMed)

Abstract
Isoxazoline insecticides, such as fluralaner (formerly A1443), are noncompetitive -aminobutyric acid (GABA) receptor (GABA-R) antagonists with selective toxicity for insects versus mammals. The isoxazoline target in house fly ( Musca domestica ) brain has subnanomolar affinity for [3H]fluralaner and a unique pattern of sensitivity to isoxazolines and avermectin B(1a) (AVE) but not to fipronil and -endosulfan. Inhibitor specificity profiles for 15 isoxazolines examined with Musca GABA-R and [3H]fluralaner, [3H]-4'-ethynyl-4-n-propylbicycloorthobenzoate ([3H]EBOB), and [3H]AVE binding follow the same structure-activity trends although without high correlation. The 3 most potent of the 15 isoxazolines tested in Musca [3H]fluralaner, [3H]EBOB, and [3H]AVE binding assays and in honeybee (Apis mellifera) brain [3H]fluralaner assays are generally those most toxic to Musca and four agricultural pests. Fluralaner does not inhibit [3H]EBOB binding to the human GABA-R recombinant β3 homopentamer, which is highly sensitive to all of the commercial GABAergic insecticides. The unique isoxazoline binding site may resurrect the GABA-R as a major insecticide target.

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