首页> 美国卫生研究院文献>PLoS Pathogens >Identification and Functional Expression of a Glutamate- and Avermectin-Gated Chloride Channel from Caligus rogercresseyi a Southern Hemisphere Sea Louse Affecting Farmed Fish
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Identification and Functional Expression of a Glutamate- and Avermectin-Gated Chloride Channel from Caligus rogercresseyi a Southern Hemisphere Sea Louse Affecting Farmed Fish

机译:来自南半球影响养殖鱼类的罗格斯(Calgus rogercresseyi)谷氨酸和阿维菌素门控氯离子通道的鉴定和功能表达

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摘要

Parasitic sea lice represent a major sanitary threat to marine salmonid aquaculture, an industry accounting for 7% of world fish production. Caligus rogercresseyi is the principal sea louse species infesting farmed salmon and trout in the southern hemisphere. Most effective control of Caligus has been obtained with macrocyclic lactones (MLs) ivermectin and emamectin. These drugs target glutamate-gated chloride channels (GluCl) and act as irreversible non-competitive agonists causing neuronal inhibition, paralysis and death of the parasite. Here we report the cloning of a full-length CrGluClα receptor from Caligus rogercresseyi. Expression in Xenopus oocytes and electrophysiological assays show that CrGluClα is activated by glutamate and mediates chloride currents blocked by the ligand-gated anion channel inhibitor picrotoxin. Both ivermectin and emamectin activate CrGluClα in the absence of glutamate. The effects are irreversible and occur with an EC50 value of around 200 nM, being cooperative (nH = 2) for ivermectin but not for emamectin. Using the three-dimensional structure of a GluClα from Caenorabditis elegans, the only available for any eukaryotic ligand-gated anion channel, we have constructed a homology model for CrGluClα. Docking and molecular dynamics calculations reveal the way in which ivermectin and emamectin interact with CrGluClα. Both drugs intercalate between transmembrane domains M1 and M3 of neighbouring subunits of a pentameric structure. The structure displays three H-bonds involved in this interaction, but despite similarity in structure only of two these are conserved from the C. elegans crystal binding site. Our data strongly suggest that CrGluClα is an important target for avermectins used in the treatment of sea louse infestation in farmed salmonids and open the way for ascertaining a possible mechanism of increasing resistance to MLs in aquaculture industry. Molecular modeling could help in the design of new, more efficient drugs whilst functional expression of the receptor allows a first stage of testing of their efficacy.
机译:寄生海虱是海洋鲑鱼养殖的主要卫生威胁,该行业占世界鱼类产量的7%。罗格斯罗格斯(Caligs rogercresseyi)是南半球养殖鲑鱼和鳟鱼的主要海虱物种。使用大环内酯(MLs)伊维菌素和Emamectin获得了对Caligus的最有效控制。这些药物靶向谷氨酸门控氯离子通道(GluCl),并作为不可逆的非竞争性激动剂,引起神经元抑制,瘫痪和寄生虫死亡。在这里,我们报道了从Caligus rogercresseyi全长CrGluClα受体的克隆。在非洲爪蟾卵母细胞中的表达和电生理分析表明,CrGluClα被谷氨酸激活,并介导被配体门控的阴离子通道抑制剂微毒素阻断的氯电流。在不存在谷氨酸的情况下,伊维菌素和埃莫菌素均激活CrGluClα。这种作用是不可逆的,在EC50值约为200 nM时发生,对于伊维菌素是协同作用(nH = 2),而对伊莫菌素则不起作用。利用秀丽隐杆线虫的GluClα的三维结构(唯一可用于任何真核配体门控阴离子通道),我们构建了CrGluClα的同源性模型。对接和分子动力学计算揭示了伊维菌素和阿莫菌素与CrGluClα相互作用的方式。两种药物都插入五聚体结构的相邻亚基的跨膜结构域M1和M3之间。该结构显示了参与此相互作用的三个氢键,但尽管结构相似,但从秀丽隐杆线虫晶体结合位点保守了两个。我们的数据强烈表明,CrGluClα是用于阿维菌素治疗养殖鲑鱼海虱侵袭的重要靶标,并为确定增加水产养殖业对ML的抗性的可能机制开辟了道路。分子建模可以帮助设计新的,更有效的药物,而受体的功能性表达可以对其功效进行测试的第一阶段。

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