Glutamate receptor inhibitors as potential insecticides

Abstract

Philanthotoxin (PhTX) is a neurotoxic constituent of the paralytic venom of the digger wasp, Philanthus triangulum. PhTX inhibits glutamate receptors of insect muscles mostly as a channel blocker, thereby producing muscle paralysis. Since glutamate receptor blockers may be of value as selective insect control agents, numerous derivatives of Ph TX were synthesized and tested for their potencies as inhibitors of insect skeletal muscle glutamate receptors. Structure‐activity relationship studies revealed that shortening the polyamine chain length reduced potency, and quaternarization of the nitrogen destroyed it. The potency was increased by a bulky anchoring group with moderate hydrophobicity at the end of the polyamine chain. The conversion of the tryosyl moiety to 3,5‐diiodo‐tyrosyl also increased potency and so did lengthening the butyryl chain from 4 to 10 carbons. Not only did Ph TXs inhibit different subtypes of glutamate receptors, including the mammalian N‐methyl‐D‐aspartate receptor, but also nicotinic receptors of insects and vertebrates. Because of this low selectively, and the hydrophilicity of the derivatives tested, which interferes with their penetration to the target receptor, these compounds cannot be used as insecticides. Nevertheless, the insect skeletal muscle glutamate receptor is a viable target for selective insecticides and major changes in Ph TX structure may possibly produce derivatives that can be potential insecticides.