首页> 外文OA文献 >Glutamate-gated chloride channels of Haemonchus contortus restore drug sensitivity to ivermectin resistant Caenorhabditis elegans.
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Glutamate-gated chloride channels of Haemonchus contortus restore drug sensitivity to ivermectin resistant Caenorhabditis elegans.

机译:捻转血矛线虫的谷氨酸盐控氯通道恢复了对伊维菌素抗性秀丽隐杆线虫的药物敏感性。

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摘要

Anthelmintic resistance is a major problem in livestock farming, especially of small ruminants, but our understanding of it has been limited by the difficulty in carrying out functional genetic studies on parasitic nematodes. An important nematode infecting sheep and goats is Haemonchus contortus; in many parts of the world this species is resistant to almost all the currently available drugs, including ivermectin. It is extremely polymorphic and to date it has proved impossible to relate any sequence polymorphisms to its ivermectin resistance status. Expression of candidate drug-resistance genes in Caenorhabditis elegans could provide a convenient means to study the effects of polymorphisms found in resistant parasites, but may be complicated by differences between the gene families of target and model organisms. We tested this using the glutamate-gated chloride channel (GluCl) gene family, which forms the ivermectin drug target and are candidate resistance genes. We expressed GluCl subunits from C. elegans and H. contortus in a highly resistant triple mutant C. elegans strain (DA1316) under the control of the avr-14 promoter; expression of GFP behind this promoter recapitulated the pattern previously reported for avr-14. Expression of ivermectin-sensitive subunits from both species restored drug sensitivity to transgenic worms, though some quantitative differences were noted between lines. Expression of an ivermectin-insensitive subunit, Hco-GLC-2, had no effect on drug sensitivity. Expression of a previously uncharacterised parasite-specific subunit, Hco-GLC-6, caused the transgenic worms to become ivermectin sensitive, suggesting that this subunit also encodes a GluCl that responds to the drug. These results demonstrate that both orthologous and paralogous subunits from C. elegans and H. contortus are able to rescue the ivermectin sensitivity of mutant C. elegans, though some quantitative differences were observed between transgenic lines in some assays. C. elegans is a suitable system for studying parasitic nematode genes that may be involved in drug resistance.
机译:驱虫抗药性是畜牧业特别是小型反刍动物的一个主要问题,但由于对寄生线虫进行功能遗传研究的困难,我们对它的理解受到限制。感染绵羊和山羊的一种重要的线虫是捻转血矛线虫。在世界许多地方,该物种对几乎所有目前可用的药物都有抗药性,包括伊维菌素。它具有极高的多态性,迄今为止,已证明不可能将任何序列多态性与其伊维菌素抗性状态相关联。在秀丽隐杆线虫中表达候选药物抗性基因可以为研究在抗性寄生虫中发现的多态性的影响提供方便的手段,但是可能由于靶标和模型生物的基因家族之间的差异而变得复杂。我们使用谷氨酸门控氯化物通道(GluCl)基因家族对其进行了测试,该基因家族形成了伊维菌素药物靶标,并且是候选耐药基因。我们在avr-14启动子的控制下,在高抗性三重突变线虫线虫菌株(DA1316)中表达了秀丽隐杆线虫和捻转线虫的GluCl亚基。在该启动子后面的GFP表达概括了先前报道的avr-14的模式。尽管两个品系之间存在一些定量差异,但两种物种的伊维菌素敏感性亚基的表达恢复了对转基因蠕虫的药物敏感性。伊维菌素不敏感亚基Hco-GLC-2的表达对药物敏感性没有影响。以前未鉴定的寄生虫特异性亚基Hco-GLC-6的表达使转基因蠕虫变得对伊维菌素敏感,这表明该亚基还编码了对药物有反应的GluCl。这些结果表明,尽管在某些测定中在转基因品系之间观察到了一些定量差异,但秀丽隐杆线虫和弯曲弯曲杆菌的直系同源和旁系亚基均能够挽救突变体秀丽隐杆线虫的伊维菌素敏感性。秀丽隐杆线虫是用于研究可能与药物抗性有关的寄生线虫基因的合适系统。

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