首页> 外文期刊>Antimicrobial agents and chemotherapy. >Interrogation of related clinical pan-azole-resistant Aspergillus fumigatus strains: G138C, Y431C, and G434C single nucleotide polymorphisms in cyp51A, upregulation of cyp51A, and integration and activation of transposon Atf1 in the cyp51A promoter.
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Interrogation of related clinical pan-azole-resistant Aspergillus fumigatus strains: G138C, Y431C, and G434C single nucleotide polymorphisms in cyp51A, upregulation of cyp51A, and integration and activation of transposon Atf1 in the cyp51A promoter.

机译:审讯相关的临床抗泛唑类烟曲霉菌株:cyp51A中的G138C,Y431C和G434C单核苷酸多态性,cyp51A的上调以及cyp51A启动子中转座子Atf1的整合和激活。

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摘要

Multiple Aspergillus fumigatus isolates from a patient with two aspergillomas complicating chronic pulmonary aspergillosis were pan-azole resistant. Microsatellite typing was identical for all isolates despite major phenotypic and some growth rate differences. Three different cyp51A mutations were found (G138C, Y431C, and G434C), of which the first two were demonstrated by heterologous expression in a hypersusceptible Saccharomyces cerevisiae strain to be at least partly responsible for elevated MICs. cyp51A and cyp51B gene duplication was excluded, but increased expression of cyp51A was demonstrated in three isolates selected for additional study (7-to 13-fold increases). In the isolate with the greatest cyp51A expression, an Aft1 transposon was found inserted 370 bp upstream of the start codon of the cyp51A gene, an integration location never previously demonstrated in Aspergillus. Two transcription start sites were identified at 49 and 136 bp upstream of the start codon. The role of the Aft1 transposon, if any, in modulating cyp51A expression remains to be established. Increased mRNA expression of the transporters AfuMDR1 and AfuMDR4 also was demonstrated in some isolates, which could contribute to azole resistance or simply represent a stress response. The diversity of confirmed and possible azole resistance mechanisms demonstrated in a single series of isogenic isolates is remarkable, indicating the ability of A. fumigatus to adapt in the clinical setting.
机译:患有两个并发慢性肺曲霉病的曲霉病患者的多个烟曲霉分离株具有泛唑耐药性。尽管主要表型和某些生长率差异,所有分离株的微卫星分型都是相同的。发现了三种不同的cyp51A突变(G138C,Y431C和G434C),其中前两种通过高敏感性酿酒酵母菌株中的异源表达证明至少部分与MIC升高有关。排除了cyp51A和cyp51B基因的重复,但是在另外3个分离株中证实了cyp51A的表达增加(增加了7至13倍)。在具有最大cyp51A表达的分离物中,发现Aft1转座子插入到cyp51A基因起始密码子上游370 bp处,这是以前未在曲霉中证实的整合位置。在起始密码子上游49和136 bp处鉴定出两个转录起始位点。 Aft1转座子,如果有的话,在调节cyp51A表达中的作用还有待确定。在某些分离物中还证明了转运蛋白AfuMDR1和AfuMDR4的mRNA表达增加,这可能促进了唑的抗性或仅表示应激反应。在一系列同基因分离物中证明的已证实的和可能的唑耐药机制的多样性非常显着,表明烟曲霉在临床环境中具有适应能力。

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