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Using Aspergillus nidulans To Identify Antifungal Drug Resistance Mutations

机译:使用构巢曲霉鉴定抗真菌药物耐药性突变

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Systemic fungal infections contribute to at least 10% of deaths in hospital settings. Most antifungal drugs target ergosterol (polyenes) or its biosynthetic pathway (azoles and allylamines), or beta-glucan synthesis (echinocandins). Antifungal drugs that target proteins are prone to the emergence of resistant strains. Identification of genes whose mutations lead to targeted resistance can provide new information on those pathways. We used Aspergillus nidulans as a model system to exploit its tractable sexual cycle and calcofluor white as a model antifungal agent to cross-reference our results with other studies. Within 2 weeks from inoculation on sublethal doses of calcofluor white, we isolated 24 A. nidulans adaptive strains from sectoring colonies. Meiotic analysis showed that these strains had single-gene mutations. In each case, the resistance was specific to calcofluor white, since there was no cross-resistance to caspofungin (echinocandin). Mutation sites were identified in two mutants by next-generation sequencing. These were confirmed by reengineering the mutation in a wild-type strain using a gene replacement strategy. One of these mutated genes was related to cell wall synthesis, and the other one was related to drug metabolism. Our strategy has wide application for many fungal species, for antifungal compounds used in agriculture as well as health care, and potentially during protracted drug therapy once drug resistance arises. We suggest that our strategy will be useful for keeping ahead in the drug resistance arms race.
机译:在医院中,全身性真菌感染导致至少10%的死亡。大多数抗真菌药物的目标是麦角固醇(多烯)或其生物合成途径(唑和烯丙胺)或β-葡聚糖合成(棘皮菌素)。靶向蛋白质的抗真菌药物容易出现耐药菌株。鉴定其突变导致靶向耐药的基因可以提供有关这些途径的新信息。我们使用构巢曲霉(Aspergillus nidulans)作为模型系统来利用其易处理的性周期,并使用钙氟荧光白(cacofluor white)作为模型抗真菌剂来交叉引用我们的结果与其他研究。在接种亚致死剂量的钙荧光白后2周内,我们从扇形菌落中分离了24株构巢曲霉适应性菌株。减数分裂分析表明这些菌株具有单基因突变。在每种情况下,由于对卡泊芬净(棘皮菌素)没有交叉抗性,因此该电阻对钙氟荧光白具有特异性。通过下一代测序在两个突变体中鉴定出突变位点。这些通过使用基因替代策略对野生型菌株中的突变进行了改造而得到证实。这些突变基因中的一个与细胞壁合成有关,另一个与药物代谢有关。我们的策略已广泛应用于许多真菌物种,用于农业以及医疗保健的抗真菌化合物,并且一旦出现耐药性,就有可能在长期药物治疗期间使用。我们建议,我们的策略将有助于在抗药性军备竞赛中保持领先地位。

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