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首页> 外文期刊>Journal of Clinical Microbiology >Clinical Significance and Phylogenetic Relationship of Novel Australian Pneumocystis jirovecii Genotypes
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Clinical Significance and Phylogenetic Relationship of Novel Australian Pneumocystis jirovecii Genotypes

机译:新型澳大利亚肺孢菌jirovecii基因型的临床意义和亲缘关系。

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Pneumocystis jirovecii is an important opportunistic pathogen in immunocompromised patients. Molecular typing is employed to study this pathogen, as no culture system exists. No Australian P. jirovecii strains have been previously studied. Direct sequencing, targeting the internal transcribed spacer (ITS) regions of the nuclear rRNA operon, the mitochondrial large-subunit rRNA (mt LSU rRNA), and the dihydropteroate synthase (DHPS) gene, was performed on 68 Australian samples, collected between 2001 and 2007. Seven novel Australian ITS haplotypes (a composite of the ITS1 and ITS2 regions) were identified (SYD1m, SYD1g, Isyd2, Esyd3, Osyd4, Ag, and Hc). A dendrogram of published ITS haplotypes revealed that of the seven novel haplotypes, three (SYD1m, SYD1g, and Osyd4) are closely related to the haplotype Eg. Applying statistical parsimony, an Australian haplotype network was constructed which identified Eg as the ancestral haplotype, with two unresolved loops encountered. This suggests that the ITS lacks the resolution required for evolutionary analysis. Only two mt LSU rRNA genotypes were detected, with genotype 1 predominating. Mutant DHPS genotypes were present in 13% (8/60) of the samples. The novel haplotype Isyd2 was associated with less severe disease than the other Australian haplotypes. In contrast, patients with mutant DHPS genotypes were more likely to have severe disease, require invasive ventilation, and have a poor outcome than patients with wild-type DHPS genotypes. In conclusion, genetic clinical correlates continue to be found for Pneumocystis pneumonia; however, they remain controversial and warrant further study.
机译:吉氏肺孢子虫是免疫功能低下患者的重要机会病原体。由于不存在培养系统,因此采用分子分型研究该病原体。没有澳大利亚 P。 jirovecii 菌株已经过研究。针对2001年至2005年之间收集的68份澳大利亚样本进行了直接测序,靶向核rRNA操纵子的内部转录间隔区(ITS),线粒体大亚基rRNA(mt LSU rRNA)和二氢蝶呤合酶(DHPS)基因。 2007。确定了七个新的澳大利亚ITS单倍型(ITS1和ITS2区域的组合)(SYD1m,SYD1g,Isyd2,Esyd3,Osyd4,Ag和Hc)。已发布的ITS单倍型的树状图显示,在七个新的单倍型中,三个(SYD1m,SYD1g和Osyd4)与单倍型Eg密切相关。应用统计简约性,构建了澳大利亚单倍型网络,该网络将Eg识别为祖先单倍型,并遇到两个未解决的环。这表明ITS缺乏进化分析所需的分辨率。仅检测到两种mt LSU rRNA基因型,其中基因型1占主导。突变的DHPS基因型存在于13%(8/60)的样本中。与澳大利亚的其他单体型相比,新型单体型Isyd2与严重程度较低的疾病相关。相反,具有突变型DHPS基因型的患者比具有野生型DHPS基因型的患者更有可能患有严重的疾病,需要有创通气并且结局较差。结论:肺囊虫肺炎的遗传临床相关性继续存在;但是,它们仍然存在争议,值得进一步研究。

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