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通过线虫运动试验对药物重利用文库进行筛选,鉴定出对牛食道口线虫和其他反刍动物寄生虫有前景的驱虫活性物质。

Screening of a drug repurposing library with a nematode motility assay identifies promising anthelmintic hits against Cooperia oncophora and other ruminant parasites.

作者信息

Liu Maoxuan, Landuyt Bart, Klaassen Hugo, Geldhof Peter, Luyten Walter

机构信息

Center of antibody drug, Institute of biomedicine and biotechnology, Shenzhen institutes of advanced technology, Chinese Academy of Science, Shenzhen, 518055, China; Department of Biology, Animal Physiology and Neurobiology Section, KU Leuven, Naamsestraat 59, box 2465, 3000 Leuven, Belgium; Department of Pharmaceutical and Pharmacological Sciences, KU Leuven, Herestraat 49, box 921, 3000 Leuven, Belgium.

Department of Biology, Animal Physiology and Neurobiology Section, KU Leuven, Naamsestraat 59, box 2465, 3000 Leuven, Belgium.

出版信息

Vet Parasitol. 2019 Jan;265:15-18. doi: 10.1016/j.vetpar.2018.11.014. Epub 2018 Dec 7.

Abstract

Parasitic nematodes continue to cause significant economic losses in livestock globally. Given the limited number of anthelmintic drugs on the market and the currently increasing drug resistance, there is an urgent need for novel anthelmintics. Most motility assays of anthelmintic activity for parasitic nematodes are laborious and low throughput, and therefore not suitable for screening large compound libraries. Cooperia oncophora accounts for a large proportion of reports on the drug-resistance development of parasites globally. Therefore, using a WMicroTracker instrument, we established a practical, automated and low-cost whole-organism motility assay against exsheathed L3 stages (xL3s) of the ruminant parasite Cooperia oncophora, and screened a repurposing library comprising 2745 molecules. Fourteen known anthelmintics contained in this library were picked up in this blind screen, as well as four novel hits: thonzonium bromide, NH125, physostigmine sulfate, and EVP4593. The four hits were also active against xL3s of Ostertagia ostertagi, Haemonchus contortus and Teladorsagia circumcincta using the same assay. Cytotoxicity testing showed that thonzonium bromide and NH125 (1-Benzyl-3-cetyl-2-methylimidazolium iodide) have significant cytotoxicity. EVP4593 (N(4)-(2-(4-phenoxyphenyl)ethyl)-4,6-quinazolinediamine) demonstrated a potent and broad anthelmintic activity, and a high selectivity index. Moreover, given its novel and unexplored chemical scaffold for anthelmintic activity, EVP4593 is an interesting anthelmintic hit for further optimization.

摘要

寄生线虫继续在全球范围内给家畜造成重大经济损失。鉴于市场上驱虫药物数量有限且目前耐药性不断增加,迫切需要新型驱虫药。大多数针对寄生线虫驱虫活性的运动性测定方法既费力又通量低,因此不适用于筛选大型化合物库。在全球寄生虫耐药性发展的报告中,牛食道口线虫占了很大比例。因此,我们使用WMicroTracker仪器,针对反刍动物寄生虫牛食道口线虫的脱鞘第三期幼虫(xL3s)建立了一种实用、自动化且低成本的全生物体运动性测定方法,并筛选了一个包含2745个分子的重新利用库。在这次盲筛中,该库中包含的14种已知驱虫药被筛选出来,还有4个新的活性物质:溴噻宗铵、NH125、硫酸毒扁豆碱和EVP4593。使用相同的测定方法,这4个活性物质对奥氏奥斯特线虫、捻转血矛线虫和环纹食道口线虫的xL3s也有活性。细胞毒性测试表明,溴噻宗铵和NH125(1-苄基-3-十六烷基-2-甲基碘化咪唑)具有显著的细胞毒性。EVP4593(N(4)-(2-(4-苯氧基苯基)乙基)-4,6-喹唑啉二胺)表现出强大且广泛的驱虫活性以及高选择性指数。此外,鉴于其具有用于驱虫活性的新型且未被探索的化学骨架,EVP4593是一个值得进一步优化的有趣的驱虫活性物质。

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