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首页> 外文期刊>International Journal for Parasitology: Drugs and Drug Resistance >Motility in the L3 stage is a poor phenotype for detecting and measuring resistance to avermectin/milbemycin drugs in gastrointestinal nematodes of livestock
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Motility in the L3 stage is a poor phenotype for detecting and measuring resistance to avermectin/milbemycin drugs in gastrointestinal nematodes of livestock

机译:L3期的运动性较弱,无法检测和测量家畜胃肠道线虫对阿维菌素/米尔贝霉素药物的耐药性

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Motility is a commonly used in vitro phenotype for assessing anthelmintic activity of candidate compounds, and for detecting anthelmintic resistance in nematodes. Third-stage larvae (L3) of parasitic nematodes are commonly used in motility-based assays because L3 are simple to obtain and can remain viable in storage for extended periods. To improve the measurement of motility of microscopic stages of nematodes, our laboratory developed the Worminator, which quantitatively measures motility of parasites. Using the Worminator, we compared the dose-response characteristics of several avermectin/milbemycin (AM) compounds using L3 from both AM-susceptible and AM-resistant Cooperia spp. (abamectin, doramectin, eprinomectin, ivermectin, moxidectin) and Haemonchus contortus (eprinomectin, ivermectin, moxidectin). Concentrations tested with the Worminator ranged from 0.156 to 40?μM. Differences in EC50 between AM-susceptible and AM-resistant isolates of Cooperia spp. and Haemonchus contortus were small, with resistance ratios ranging from 1.00 to 1.34 for Cooperia spp., 0.99 to 1.65 for Haemonchus contortus. Larval migration inhibition assays were conducted using the same isolates and were equally ineffective for detection of resistance with resistance ratios less than 2.0. These results contrast with those of the Larval Development Assay where we obtained a resistance ratio of 16.48 using the same isolates of Haemonchus contortus. Moreover, even at the highest concentration tested (40 μM), 100% inhibition of motility was never achieved and EC50 for Worminator assays were more than 100× higher than peak plasma levels achieved in vivo following treatment. These data demonstrate that dose-response characteristics for inhibition of motility in L3 of gastrointestinal nematodes of livestock do not significantly differ for AM-susceptible and AM-resistant isolates. These data challenge the suitability of motility as a phenotype for detecting and measuring resistance to AM drugs in gastrointestinal nematodes of livestock.
机译:运动性是一种常用的体外表型,用于评估候选化合物的驱虫活性,并用于检测线虫的驱虫抗性。寄生线虫的第三级幼虫(L3)通常用于基于运动性的测定中,因为L3易于获得并且可以长期保存。为了改善线虫微观阶段的活力测量,我们的实验室开发了Worminator,它可以定量测量寄生虫的活力。使用促生物降解剂,我们使用AM易感性和AM抗性库珀属的L3比较了几种阿维菌素/米尔贝霉素(AM)化合物的剂量反应特性。 (阿维菌素,多拉菌素,依普诺菌素,伊维菌素,莫昔克丁)和捻转血Haemonchus contortus(依普诺菌素,依维菌素,莫昔克丁)。用Worminator测试的浓度范围为0.156至40?M。 Cooperia spp的AM敏感菌和AM抵抗菌之间EC 50 的差异。鸡和鸡爪蟾的变小,对Cooperia spp。的抗性比在1.00至1.34之间,对鸡爪蟹的抗性比率在0.99至1.65之间。使用相同的分离物进行幼虫迁移抑制试验,对于耐药率小于2.0的耐药性检测同样无效。这些结果与幼虫发育试验的结果相反,在幼虫发育试验中,我们使用相同的捻转血矛线虫菌株获得了16.48的抗性比。此外,即使在最高测试浓度(40μM)下,也从未实现对运动的100%抑制,并且对于Worminator分析,EC 50 比治疗后体内达到的峰值血浆水平高100倍以上。这些数据表明,对于AM易感和AM耐药菌株,抑制家畜胃肠道线虫L3活力的剂量反应特性没有显着差异。这些数据挑战了以运动性为表型来检测和测量家畜胃肠线虫对AM药物的耐药性的适用性。

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