首页> 外文期刊>European journal of clinical microbiology and infectious diseases: Official publication of the European Society of Clinical Microbiology >Species distribution and susceptibility profile to fluconazole, voriconazole and MXP-4509 of 551 clinical yeast isolates from a Romanian multi-centre study
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Species distribution and susceptibility profile to fluconazole, voriconazole and MXP-4509 of 551 clinical yeast isolates from a Romanian multi-centre study

机译:罗马尼亚多中心研究的551种临床酵母菌株对氟康唑,伏立康唑和MXP-4509的物种分布和敏感性分布

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This is the first multi-centre study regarding yeast infections in Romania. The aim was to determine the aetiological spectrum and susceptibility pattern to fluconazole, voriconazole and the novel compound MXP-4509. The 551 isolates were identified using routine laboratory methods, matrix-assisted laser desorption ionisation time-of-flight mass spectrometry (MALDI-TOF MS) and DNA sequence analysis. Susceptibility testing was performed using the European Committee for Antimicrobial Susceptibility Testing (EUCAST) method and breakpoints. The yeasts originated from superficial infections (SUP, 51.5 %), bloodstream infections (BSI, 31.6 %) and deep-seated infections (DEEP, 16.9 %), from patients of all ages. Nine genera and 30 species were identified. The 20 Candida species accounted for 94.6 % of all isolates. C. albicans was the overall leading pathogen (50.5 %). Lodderomyces elongisporus is reported for the first time as a fungaemia cause in Europe. C. glabrata and Saccharomyces cerevisiae, as well as the non-Candida spp. and non-albicans Candida spp. groups, showed decreased fluconazole susceptibility (< 75 %). The overall fluconazole resistance was 10.2 %. C. krusei accounted for 27 of the 56 fluconazole-resistant isolates. The overall voriconazole resistance was 2.5 % and was due mainly to C. glabrata and C. tropicalis isolates. Fluconazole resistance rates for the three categories of infection were similar to the overall value; voriconazole resistance rates differed: 4 % for BSI, 3.2 % for DEEP and 1.4 % for SUP. The antifungal activity of MXP-4509 was superior to voriconazole against C. glabrata and many fluconazole-resistant isolates. There was a large percentage of non-albicans Candida isolates. A large part of the high fluconazole resistance was not acquired but intrinsic, resulting from the high percentage of C. krusei.
机译:这是罗马尼亚第一个关于酵母菌感染的多中心研究。目的是确定对氟康唑,伏立康唑和新型化合物MXP-4509的病原谱和敏感性模式。使用常规实验室方法,基质辅助激光解吸电离飞行时间质谱(MALDI-TOF MS)和DNA序列分析鉴定了551个分离株。药敏试验是使用欧洲抗菌药敏试验委员会(EUCAST)方法和断点进行的。酵母菌起源于各个年龄段的患者,均来自浅表感染(SUP,占51.5%),血流感染(BSI,占31.6%)和深部感染(DEEP,占16.9%)。确定了九属和30种。 20个念珠菌属占所有分离株的94.6%。白色念珠菌是总的主要病原体(50.5%)。在欧洲,首次报道了长形假单胞菌是真菌病的原因。 C. glabrata和酿酒酵母,以及非Candida spp。和非白色念珠菌。组显示氟康唑敏感性降低(<75%)。氟康唑的总耐药率为10.2%。克鲁维梭菌占耐氟康唑的56种分离株中的27种。伏立康唑的总体耐药率为2.5%,主要归因于光滑念珠菌和热带念珠菌的分离。氟康唑对这三类感染的耐药率与总值相似。伏立康唑的耐药率有所不同:BSI为4%,DEEP为3.2%,SUP为1.4%。 MXP-4509的抗真菌活性优于伏立康唑,对光滑毛囊梭菌和许多耐氟康唑的菌株均无害。有大量非白色念珠菌分离株。高氟康唑耐药性的很大一部分不是固有的,而是内在的,这是由于克鲁斯梭菌的高百分比所致。

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