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在体外对捻转血矛线虫幼虫阶段施加左旋咪唑选择压力九代后,会产生耐药性,且仅在幼虫早期阶段出现特定的靶位点基因表达变化。

In vitro levamisole selection pressure on larval stages of Haemonchus contortus over nine generations gives rise to drug resistance and target site gene expression changes specific to the early larval stages only.

作者信息

Sarai Ranbir S, Kopp Steven R, Knox Malcolm R, Coleman Glen T, Kotze Andrew C

机构信息

CSIRO Agriculture Flagship, 306 Carmody Rd, St Lucia, Brisbane, QLD 4067, Australia; School of Veterinary Science, University of Queensland, Gatton, QLD 4341, Australia.

School of Veterinary Science, University of Queensland, Gatton, QLD 4341, Australia.

出版信息

Vet Parasitol. 2015 Jun 30;211(1-2):45-53. doi: 10.1016/j.vetpar.2015.05.002. Epub 2015 May 8.

DOI:10.1016/j.vetpar.2015.05.002
PMID:25983232
Abstract

There is some evidence that resistance to levamisole and pyrantel in trichostrongylid nematodes is due to changes in the composition of nicotinic acetylcholine receptors (nAChRs) which represent the drug target site. Altered expression patterns of genes coding for nAChR subunits, as well as the presence of truncated versions of several subunits, have been implicated in observed resistances. The studies have mostly compared target sites in worm isolates of very different genetic background, and hence the ability to associate the molecular changes with drug sensitivity alone have been clouded to some extent. The present study aimed to circumvent this issue by following target site gene expression pattern changes as resistance developed in Haemonchus contortus worms under laboratory selection pressure with levamisole. We applied drug selection pressure to early stage larvae in vitro over nine generations, and monitored changes in larval and adult drug sensitivities and target site gene expression patterns. High level resistance developed in larvae, with resistance factors of 94-fold and 1350-fold at the IC50 and IC95, respectively, in larval development assays after nine generations of selection. There was some cross-resistance to bephenium (70-fold increase in IC95). The expression of all the putative subunit components of levamisole-sensitive nAChRs, as well as a number of ancillary protein genes, particularly Hco-unc-29.1 and -ric-3, were significantly decreased (up to 5.5-fold) in the resistant larvae at generation nine compared to the starting population. However, adult worms did not show any resistance to levamisole, and showed an inverse pattern of gene expression changes, with many target site genes showing increased expression compared to the starting population. A comparison of the larval/adult drug sensitivity data with the known relationships for field-derived isolates indicated that the adults of our selected population should have been highly resistant to the drug if the larval/adult sensitivity relationships were in accordance with previous field isolates. Hence, our selected worms showed a life-stage drug sensitivity pattern quite different to that seen in the field. The present study has highlighted an association between drug target site changes and resistance to levamisole in H. contortus larvae. However, it has also highlighted the artificial nature of the larval selection method with levamisole, as the resistance phenotype and the associated molecular changes were only observed in the drug-pressured life stage. The study therefore reinforces the need for caution in extrapolating larval-based laboratory selection outcomes to field resistances.

摘要

有证据表明,毛圆科线虫对左旋咪唑和噻嘧啶的抗性是由于作为药物作用靶点的烟碱型乙酰胆碱受体(nAChRs)组成发生了变化。编码nAChR亚基的基因表达模式改变,以及几个亚基截短形式的存在,都与观察到的抗性有关。这些研究大多比较了遗传背景差异很大的蠕虫分离株中的靶点,因此,仅将分子变化与药物敏感性联系起来的能力在一定程度上受到了影响。本研究旨在通过跟踪在左旋咪唑实验室选择压力下捻转血矛线虫抗性发展过程中靶点基因表达模式的变化来规避这个问题。我们在体外对早期幼虫施加药物选择压力,持续九代,并监测幼虫和成虫的药物敏感性以及靶点基因表达模式的变化。幼虫产生了高水平抗性,在经过九代选择后的幼虫发育试验中,IC50和IC95的抗性因子分别为94倍和1350倍。对苄酚宁有一定交叉抗性(IC95增加70倍)。与起始群体相比,第九代抗性幼虫中左旋咪唑敏感型nAChRs所有假定亚基成分以及一些辅助蛋白基因,特别是Hco-unc-29.1和-ric-3的表达显著降低(高达5.5倍)。然而,成虫对左旋咪唑没有表现出任何抗性,并且呈现出相反的基因表达变化模式,与起始群体相比,许多靶点基因表达增加。将幼虫/成虫药物敏感性数据与田间分离株的已知关系进行比较表明,如果幼虫/成虫敏感性关系与先前的田间分离株一致,我们所选群体的成虫应该对该药物具有高度抗性。因此,我们所选的蠕虫表现出与田间所见截然不同的生活阶段药物敏感性模式。本研究突出了药物靶点变化与捻转血矛线虫幼虫对左旋咪唑抗性之间的关联。然而,它也突出了左旋咪唑幼虫选择方法的人为性质,因为抗性表型和相关分子变化仅在受药物压力的生活阶段观察到。因此,该研究强调了在将基于幼虫的实验室选择结果外推至田间抗性时需要谨慎。

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