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鳞翅目毛毛虫产生的痛苦防御毒液的产生、组成和作用模式。

Production, composition, and mode of action of the painful defensive venom produced by a limacodid caterpillar, .

机构信息

Institute for Molecular Bioscience, The University of Queensland, St Lucia, QLD, 4072, Australia;

Institute for Molecular Bioscience, The University of Queensland, St Lucia, QLD, 4072, Australia.

出版信息

Proc Natl Acad Sci U S A. 2021 May 4;118(18). doi: 10.1073/pnas.2023815118.

Abstract

Venoms have evolved independently several times in Lepidoptera. Limacodidae is a family with worldwide distribution, many of which are venomous in the larval stage, but the composition and mode of action of their venom is unknown. Here, we use imaging technologies, transcriptomics, proteomics, and functional assays to provide a holistic picture of the venom system of a limacodid caterpillar, Contrary to dogma that defensive venoms are simple in composition, produces a complex venom containing 151 proteinaceous toxins spanning 59 families, most of which are peptides <10 kDa. Three of the most abundant families of venom peptides (vulnericins) are 1) analogs of the adipokinetic hormone/corazonin-related neuropeptide, some of which are picomolar agonists of the endogenous insect receptor; 2) linear cationic peptides derived from cecropin, an insect innate immune peptide that kills bacteria and parasites by disrupting cell membranes; and 3) disulfide-rich knottins similar to those that dominate spider venoms. Using venom fractionation and a suite of synthetic venom peptides, we demonstrate that the cecropin-like peptides are responsible for the dominant pain effect observed in mammalian in vitro and in vivo nociception assays and therefore are likely to cause pain after natural envenomations by Our data reveal convergent molecular evolution between limacodids, hymenopterans, and arachnids and demonstrate that lepidopteran venoms are an untapped source of novel bioactive peptides.

摘要

鳞翅目昆虫的毒液经历了多次独立进化。长鼻目是一个世界性分布的科,其中许多幼虫阶段是有毒的,但它们毒液的组成和作用方式尚不清楚。在这里,我们使用成像技术、转录组学、蛋白质组学和功能分析,为长鼻目毛虫的毒液系统提供了一个全面的图景。与防御性毒液组成简单的教条相反,这种毛毛虫产生了一种复杂的毒液,其中含有 151 种蛋白毒素,跨越 59 个家族,其中大多数肽小于 10 kDa。毒液肽中最丰富的三个家族(脆弱素)是 1) 与促前胸腺激素/心激素相关神经肽的类似物,其中一些是内源性昆虫受体的皮摩尔级激动剂;2) 来源于昆虫先天免疫肽 Cecropin 的线性阳离子肽,通过破坏细胞膜杀死细菌和寄生虫;3) 富含二硫键的 knottins 类似于那些在蜘蛛毒液中占主导地位的 knottins。我们使用毒液分级和一系列合成毒液肽,证明 Cecropin 样肽是在哺乳动物体外和体内伤害感受测定中观察到的主要疼痛效应的原因,因此在自然中毒后可能会引起疼痛。我们的数据揭示了长鼻目、膜翅目和蛛形纲动物之间的趋同分子进化,并表明鳞翅目昆虫毒液是一种未开发的新型生物活性肽来源。

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