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A recombinant fusion protein containing a spider toxin specific for the insect voltage-gated sodium ion channel shows oral toxicity towards insects of different orders

机译:含有特异于昆虫电压门控钠离子通道的蜘蛛毒素的重组融合蛋白对不同等级的昆虫表现出口服毒性

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摘要

Recombinant fusion protein technology allows specific insecticidal protein and peptide toxins to display activity in orally-delivered biopesticides. The spider venom peptide δ-amaurobitoxin-PI1a, which targets insect voltage-gated sodium channels, was fused to the “carrier” snowdrop lectin (GNA) to confer oral toxicity.The toxin itself (PI1a) and an amaurobitoxin/GNA fusion protein (PI1a/GNA) were produced using the yeast Pichia pastoris as expression host. Although both proteins caused mortality when injected into cabbage moth (Mamestra brassicae) larvae, the PI1a/GNA fusion was approximately 6 times as effective as recombinant PI1a on a molar basis. PI1a alone was not orally active against cabbage moth larvae, but a single 30 μg dose of the PI1a/GNA fusion protein caused 100% larval mortality within 6 days when fed to 3rd instar larvae, and caused significant reductions in survival, growth and feeding in 4th – 6th instar larvae. Transport of fusion protein from gut contents to the haemolymph of cabbage moth larvae, and binding to the nerve chord, was shown by Western blotting. The PI1a/GNA fusion protein also caused mortality when delivered orally to dipteran (Musca domestica; housefly) and hemipteran (Acyrthosiphon pisum; pea aphid) insects, making it a promising candidate for development as a biopesticide.
机译:重组融合蛋白技术可使特定的杀虫蛋白和肽毒素在口服生物杀虫剂中发挥活性。将靶向昆虫电压门控钠通道的蜘蛛毒肽δ-金属尿嘧啶-PI1a与“载体”雪花莲凝集素(GNA)融合,赋予口服毒性。毒素本身(PI1a)和金属尿嘧啶/ GNA融合蛋白(使用酵母毕赤酵母作为表达宿主产生PI1a / GNA)。尽管两种蛋白质在注入卷心菜蛾(Mamestra brasicae)幼虫中都会导致死亡,但按摩尔计算,PI1a / GNA融合的效力约为重组PI1a的6倍。单独的PI1a对卷心菜蛾幼虫没有口服活性,但是单剂量PI3a / GNA融合蛋白30μg喂食3龄幼虫后6天内可导致100%幼虫死亡率,并显着降低成年幼虫的存活率,生长量和摄食量4-6龄幼虫。蛋白质印迹显示融合蛋白从肠内容物转运至甘蓝蛾幼虫的血淋巴,并与神经弦结合。当将PI1a / GNA融合蛋白口服递送至双翅目昆虫(家蝇;家蝇)和半翅目昆虫(豌豆蚜;豌豆蚜)时,也会引起死亡,这使其有望成为发展为生物农药的候选者。

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