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首页> 外文期刊>Molecular & cellular proteomics: MCP >Parasitoid Jewel Wasp Mounts Multipronged Neurochemical Attack to Hijack a Host Brain
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Parasitoid Jewel Wasp Mounts Multipronged Neurochemical Attack to Hijack a Host Brain

机译:寄生珠宝黄蜂坐在多强神经化学攻中劫持宿主脑

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摘要

The parasitoid emerald jewel wasp Ampulex compressa induces a compliant state of hypokinesia in its host, the American cockroach Periplaneta americana through direct envenomation of the central nervous system (CNS). To elucidate the biochemical strategy underlying venominduced hypokinesia, we subjected the venom apparatus and milked venom to RNAseq and proteomics analyses to construct a comprehensive "venome," consisting of 264 proteins. Abundant in the venome are enzymes endogenous to the host brain, including M13 family metalloproteases, phospholipases, adenosine deaminase, hyaluronidase, and neuropeptide precursors. The amphipathic, alpha-helical ampulexins are among the most abundant venom components. Also prominent are members of the Toll/NF-kappa B signaling pathway, including proteases Persephone, Snake, Easter, and the Toll receptor ligand Spatzle. We find evidence that venom components are processed following envenomation. The acidic (pH similar to 4) venom contains unprocessed neuropeptide tachykinin and corazonin precursors and is conspicuously devoid of the corresponding processed, biologically active peptides. Neutralization of venom leads to appearance of mature tachykinin and corazonin, suggesting that the wasp employs precursors as a prolonged time-release strategy within the host brain post-envenomation. Injection of fully processed tachykinin into host cephalic ganglia elicits short-term hypokinesia. Ion channel modifiers and cytolytic toxins are absent in A. compressa venom, which appears to hijack control of the host brain by introducing a "storm" of its own neurochemicals. Our findings deepen understanding of the chemical warfare underlying host-parasitoid interactions and in particular neuromodulatory mechanisms that enable manipulation of host behavior to suit the nutritional needs of opportunistic parasitoid progeny.
机译:寄生虫翡翠宝石黄蜂琥珀般的Complex Compress在其主持人中突出了柔顺的低压因子,美国蟑螂Periplaneta Americana通过直接encenomation的中枢神经系统(CNS)。为了阐明毒液诱导的低管基础毒性的生物化学策略,我们将毒液装置与RNASEQ和蛋白质组学分析进行了毒液,并挤奶,以构建由264个蛋白质组成的综合“肠道”。静脉中的丰富是内源性对宿主脑的酶,包括M13家族金属蛋白酶,磷脂酶,腺苷脱氨酶,透明质酸酶和神经肽前体。两亲性α-螺旋氨吡脂素是最丰富的毒液组分。还突出的是Toll / NF-Kappa B信用途径的成员,包括蛋白酶Persephone,Snake,Easter和Toll受体配体Spatzle。我们发现证据表明毒液组分在encenomation之后加工。酸性(类似于4)毒液含有未加工的神经肽Tachykinin和Corazonin前体,并且具有相应的加工,生物活性肽显着地缺乏。毒液中和导致成熟的Tachykinin和Corazonin的出现,表明WASP在envengomation后宿主脑内的延长时间释放策略中使用前体。将完全加工的Tachykinin注射到宿主头脑神经节Elicits短期低压症。在A. complecta毒液中不存在离子通道改性剂和细胞溶解毒素,其通过引入其自身神经化学的“风暴”似乎劫持宿主脑的控制。我们的研究结果深化了对宿主寄生虫相互作用的潜在化学战,特别是神经调节机制,使得能够操纵宿主行为,以适应机会主义寄生虫后代的营养需求。

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    Univ Calif Riverside Grad Program Biochem &

    Mol Biol Riverside CA 92521 USA;

    Ben Guion Univ Negev Dept Life Sci Beer Sheva Israel;

    Univ Calif Riverside Dept Mol Cell &

    Syst Biol Riverside CA 92521 USA;

    Univ Calif Riverside Dept Mol Cell &

    Syst Biol Riverside CA 92521 USA;

    Univ Calif Riverside Dept Mol Cell &

    Syst Biol Riverside CA 92521 USA;

    Univ Calif Riverside Dept Mol Cell &

    Syst Biol Riverside CA 92521 USA;

    Univ Calif Riverside Dept Entomol Riverside CA 92521 USA;

    Univ Calif Riverside Inst Integrated Genome Biol Riverside CA 92521 USA;

    Univ Calif Riverside Dept Microbiol &

    Plant Pathol Riverside CA 92521 USA;

    Ben Guion Univ Negev Dept Life Sci Beer Sheva Israel;

    Univ Calif Riverside Grad Program Biochem &

    Mol Biol Riverside CA 92521 USA;

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  • 正文语种 eng
  • 中图分类 生物化学;
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