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Generality of toxins in defensive symbiosis: Ribosome-inactivating proteins and defense against parasitic wasps in Drosophila

机译:防御性共生中毒素的一般性:核糖体失活蛋白和果蝇中对寄生性黄蜂的防御

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摘要

While it has become increasingly clear that multicellular organisms often harbor microbial symbionts that protect their hosts against natural enemies, the mechanistic underpinnings underlying most defensive symbioses are largely unknown. Spiroplasma bacteria are widespread associates of terrestrial arthropods, and include strains that protect diverse Drosophila flies against parasitic wasps and nematodes. Recent work implicated a ribosome-inactivating protein (RIP) encoded by Spiroplasma, and related to Shiga-like toxins in enterohemorrhagic Escherichia coli, in defense against a virulent parasitic nematode in the woodland fly, Drosophila neotestacea. Here we test the generality of RIP-mediated protection by examining whether Spiroplasma RIPs also play a role in wasp protection, in D. melanogaster and D. neotestacea. We find strong evidence for a major role of RIPs, with ribosomal RNA (rRNA) from the larval endoparasitic wasps, Leptopilina heterotoma and Leptopilina boulardi, exhibiting the hallmarks of RIP activity. In Spiroplasma-containing hosts, parasitic wasp ribosomes show abundant site-specific depurination in the α-sarcin/ricin loop of the 28S rRNA, with depurination occurring soon after wasp eggs hatch inside fly larvae. Interestingly, we found that the pupal ectoparasitic wasp, Pachycrepoideus vindemmiae, escapes protection by Spiroplasma, and its ribosomes do not show high levels of depurination. We also show that fly ribosomes show little evidence of targeting by RIPs. Finally, we find that the genome of D. neotestacea’s defensive Spiroplasma encodes a diverse repertoire of RIP genes, which are differ in abundance. This work suggests that specificity of defensive symbionts against different natural enemies may be driven by the evolution of toxin repertoires, and that toxin diversity may play a role in shaping host-symbiont-enemy interactions.
机译:尽管越来越清楚的是,多细胞生物通常带有微生物共生体,以保护其宿主免受天敌的侵害,但大多数防御性共生体背后的机制基础在很大程度上尚不清楚。螺旋体细菌是陆生节肢动物的广泛同伴,并包括保护各种果蝇蝇免受寄生性黄蜂和线虫侵害的菌株。最近的工作涉及由螺旋体编码的核糖体失活蛋白(RIP),与肠道出血性大肠杆菌中的志贺氏样毒素有关,以防御林地蝇Drosophila neotestacea中的强力寄生线虫。在这里,我们通过检查螺旋藻RIPs在黑腹果蝇和新睾藻中是否也在黄蜂保护中发挥作用,来测试RIP介导的保护的一般性。我们发现有力的证据表明RIP具有重要作用,其幼虫内寄生性黄蜂,核小体钩端螺旋体和小核对虾钩体的核糖体RNA(rRNA)表现出RIP活性的标志。在含有螺旋体的宿主中,寄生的黄蜂核糖体在28S rRNA的α-sarcin/ ricin环中显示出丰富的特定位点去嘌呤,黄蜂卵在蝇幼虫孵化后不久就发生了去嘌呤。有趣的是,我们发现up外寄生性黄蜂Pachycrepoideus vindemmiae不受螺旋体的保护,其核糖体未显示高水平的净化。我们还表明,蝇核糖体几乎没有RIPs靶向的证据。最后,我们发现D. neotestacea's 防御性 Spiroplasma 的基因组编码了丰富多样的RIP基因。这项工作表明防御共生体对不同天敌的特异性可能是由毒素库的演变所驱动的,并且毒素多样性可能在塑造宿主-共生体-敌人的相互作用中起作用。

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