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首页> 外文期刊>Antimicrobial agents and chemotherapy. >A CTG Clade Candida Yeast Genetically Engineered for the Genotype-Phenotype Characterization of Azole Antifungal Resistance in Human-Pathogenic Yeasts
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A CTG Clade Candida Yeast Genetically Engineered for the Genotype-Phenotype Characterization of Azole Antifungal Resistance in Human-Pathogenic Yeasts

机译:CTG CTG Candida酵母遗传设计用于人致病酵母中唑脂抗原性的基因型 - 表型表征

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A strain of the opportunistic pathogenic yeast Candida lusitaniae was genetically modified for use as a cellular model for assessing by allele replacement the impact of lanosterol C14 alpha-demethylase ERG11 mutations on azole resistance. Candida lusitaniae was chosen because it is susceptible to azole antifungals, it belongs to the CTG clade of yeast, which includes most of the Candida species pathogenic for humans, and it is haploid and easily amenable to genetic transformation and molecular modeling. In this work, allelic replacement is targeted at the ERG11 locus by the reconstitution of a functional auxotrophic marker in the 3' intergenic region of ERG11. Homologous and heterologous ERG11 alleles are expressed from the resident ERG11 promoter of C. lusitaniae, allowing accurate comparison of the phenotypic change in azole susceptibility. As a proof of concept, we successfully expressed in C. lusitaniae different ERG11 alleles, either bearing or not bearing mutations retrieved from a clinical context, from two phylogenetically distant yeasts, C. albicans and Kluyveromyces marxianus. Candida lusitaniae constitutes a high-fidelity expression system, giving specific Erg11p-dependent fluconazole MICs very close to those observed with the ERG11 donor strain. This work led us to characterize the phenotypic effect of two kinds of mutation: mutation conferring decreased fluconazole susceptibility in a species-specific manner and mutation conferring fluconazole resistance in several yeast species. In particular, a missense mutation affecting amino acid K143 of Erg11p in Candida species, and the equivalent position K151 in K. marxianus, plays a critical role in fluconazole resistance.
机译:机会致病酵母念珠菌的一种菌株在遗传修饰用作通过等位基因替代评估Lanterol醇C14α-脱甲基酶ERG11突变对唑抗性的影响的细胞模型。选择了念珠菌,因为它易受唑脂肪酸的影响,它属于酵母的CTG曲线,其中包括对人类的大多数念珠菌物种致病性,并且它是单倍体,并且易于遗传转化和分子模拟。在这项工作中,通过在ERG11的3'代鼻区域中的功能性滋养缺乏标记物中重构,在ERG11基因座上靶向。同源和异源ERG11等位基因由C.Lusitaniae的驻留ERG11启动子表达,允许准确比较唑易感性的表型变化。作为概念证明,我们成功地用C. lusitaniae不同的ERG11等位基因表达,无论是轴承还是未从临床上下文中检索的突变,从两个系统源性遥远的酵母,C. albicans和Kluyveromyces Marxianus。 Candida Lusitaniae构成了一种高保真表达系统,使特定的ERG11P依赖性氟康唑掩模非常接近于用ERG11供体菌株观察的那些。这项工作导致我们表征了两种突变的表型效果:突变赋予赋予氟康唑敏感性的氟康唑敏感性和赋予几种酵母物种中的氟康唑抗性的突变。特别地,影响念珠菌物种中ERG11p的氨基酸K143的麦基突变,并在K.Marxianus的当量K151中,在氟康唑抗性中起着关键作用。

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