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多药转运蛋白和有机阴离子转运多肽可保护昆虫免受强心苷的毒性影响。

Multidrug transporters and organic anion transporting polypeptides protect insects against the toxic effects of cardenolides.

作者信息

Groen Simon C, LaPlante Erika R, Alexandre Nicolas M, Agrawal Anurag A, Dobler Susanne, Whiteman Noah K

机构信息

Department of Ecology and Evolutionary Biology, University of Arizona, Tucson, AZ 85721, USA.

Department of Ecology and Evolutionary Biology, University of Arizona, Tucson, AZ 85721, USA; Department of Integrative Biology, University of California, Berkeley, 3040 Valley Life Sciences Building, Berkeley, CA 94720, USA.

出版信息

Insect Biochem Mol Biol. 2017 Feb;81:51-61. doi: 10.1016/j.ibmb.2016.12.008. Epub 2016 Dec 21.

Abstract

In the struggle against dietary toxins, insects are known to employ target site insensitivity, metabolic detoxification, and transporters that shunt away toxins. Specialized insects across six taxonomic orders feeding on cardenolide-containing plants have convergently evolved target site insensitivity via specific amino acid substitutions in the Na/K-ATPase. Nonetheless, in vitro pharmacological experiments have suggested a role for multidrug transporters (Mdrs) and organic anion transporting polypeptides (Oatps), which may provide a basal level of protection in both specialized and non-adapted insects. Because the genes coding for these proteins are evolutionarily conserved and in vivo genetic evidence in support of this hypothesis is lacking, here we used wildtype and mutant Drosophila melanogaster (Drosophila) in capillary feeder (CAFE) assays to quantify toxicity of three chemically diverse, medically relevant cardenolides. We examined multiple components of fitness, including mortality, longevity, and LD50, and found that, while the three cardenolides each stimulated feeding (i.e., no deterrence to the toxin), all decreased lifespan, with the most apolar cardenolide having the lowest LD50 value. Flies showed a clear non-monotonic dose response and experienced high levels of toxicity at the cardenolide concentration found in plants. At this concentration, both Mdr and Oatp knockout mutant flies died more rapidly than wildtype flies, and the mutants also experienced more adverse neurological effects on high-cardenolide-level diets. Our study further establishes Drosophila as a model for the study of cardenolide pharmacology and solidifies support for the hypothesis that multidrug and organic anion transporters are key players in insect protection against dietary cardenolides.

摘要

在与饮食毒素的斗争中,已知昆虫会采用靶位点不敏感、代谢解毒以及将毒素分流的转运蛋白。以含有强心甾的植物为食的六个分类目的特殊昆虫,通过钠钾ATP酶中的特定氨基酸取代,趋同进化出了靶位点不敏感。尽管如此,体外药理学实验表明多药转运蛋白(Mdrs)和有机阴离子转运多肽(Oatps)发挥了作用,它们可能在特殊昆虫和未适应的昆虫中都提供了基础水平的保护。由于编码这些蛋白质的基因在进化上是保守的,且缺乏支持这一假设的体内遗传学证据,我们在此使用野生型和突变型黑腹果蝇,通过毛细管取食(CAFE)试验来量化三种化学性质不同、具有医学相关性的强心甾的毒性。我们检查了多个适合度指标,包括死亡率、寿命和半数致死剂量(LD50),发现虽然这三种强心甾都刺激了取食(即对毒素没有威慑作用),但它们都缩短了寿命,其中极性最小的强心甾LD50值最低。果蝇表现出明显的非单调剂量反应,在植物中发现的强心甾浓度下经历了高水平的毒性。在此浓度下,Mdr和Oatp基因敲除突变果蝇比野生型果蝇死亡更快,并且这些突变体在高强心甾水平的饮食中还经历了更严重的神经学不良影响。我们的研究进一步确立了果蝇作为强心甾药理学研究模型的地位,并巩固了对多药和有机阴离子转运蛋白是昆虫抵御饮食强心甾的关键参与者这一假设的支持。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f2a/5428987/7ee3912e114b/nihms857058f1.jpg

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