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从上海传染病患者中分离出的白色念珠菌菌株的基因和表型特征

Genetic and phenotypic characterization of Candida albicans strains isolated from infectious disease patients in Shanghai.

作者信息

Hu Lvyin, Du Xin, Li Tianming, Song Yan, Zai Shubei, Hu Xiangnan, Zhang Xiaonan, Li Min

机构信息

Department of Clinical Laboratory, Shanghai Public Health Clinical Center, Fudan University, No. 2901 Cao Lang Rd, Shanghai, PR China.

Department of Laboratory Medicine, Huashan Hospital, Shanghai Medical College, Fudan University, 12 Central Urumqi Road, Shanghai, PR China.

出版信息

J Med Microbiol. 2015 Jan;64(Pt 1):74-83. doi: 10.1099/jmm.0.080200-0. Epub 2014 Oct 28.

Abstract

Candida albicans, as an opportunistic pathogen, can cause superficial and life-threatening candidiasis in immunocompromised individuals. The formation of surface-associated biofilms and the appearance of drug resistance pose a significant challenge for clinical intervention. In this study, a total of 104 hospital-acquired C. alibcans clinical isolates were collected from sterile sites and mucosal lesions of 92 infectious disease patients in the Shanghai Public Health Clinical Center and analysed. The resistance rates to fluconazole, itraconazole and voriconazole were 12.5 %, 15.4 % and 11.5 % respectively. Multilocus sequence typing (MLST) analysis identified 63 diploid sequence types (DSTs) with a decentralized phylogeny, of which 37 DSTs (58.7 %) had not been reported in the online MLST database. Loss of heterozygosity was observed in ACC1 and ADP1 sequences obtained from six sequential isolates from a patient receiving antifungal treatment, which exemplified the effect of microevolution on C. albicans genetic alterations. Biofilm formation capability, an important virulence trait of C. albicans, was variable among strains isolated from different anatomical sites (P = 0.0302) and affected by genotypes (P = 0.0185). The mRNA levels of the azole antifungal target ERG11 gene and efflux pump genes (CDR1, CDR2 and MDR1) were detected in 9-18.1 % of azole-resistant and susceptible-dose dependent (S-DD) isolates. Twelve mutations encoding distinct amino acid substitutions in ERG11 were found in azole-resistant and S-DD isolates. Among them, A114S, Y132H and Y257H substitution in the ERG11 gene may be primarily related to azole resistance. Taken together, we observed a high level of diversity within C. albicans isolates. Multiple inter-related underlying mechanisms, including genetic and environmental factors, may account for high surface adhesion or azole resistance in clinical C. albicans infections.

摘要

白色念珠菌作为一种机会致病菌,可在免疫功能低下的个体中引起浅表性和危及生命的念珠菌病。表面相关生物膜的形成和耐药性的出现对临床干预构成了重大挑战。在本研究中,从上海公共卫生临床中心92例传染病患者的无菌部位和黏膜病变中收集了总共104株医院获得性白色念珠菌临床分离株并进行分析。对氟康唑、伊曲康唑和伏立康唑的耐药率分别为12.5%、15.4%和11.5%。多位点序列分型(MLST)分析鉴定出63种二倍体序列类型(DSTs),其系统发育呈分散状,其中37种DSTs(58.7%)在在线MLST数据库中尚未见报道。在一名接受抗真菌治疗患者的6株连续分离株获得的ACC1和ADP1序列中观察到杂合性缺失,这例证了微进化对白色念珠菌基因改变的影响。生物膜形成能力是白色念珠菌的一个重要毒力特征,在从不同解剖部位分离的菌株中存在差异(P = 0.0302),并受基因型影响(P = 0.0185)。在9% - 18.1%的唑类耐药和剂量依赖性敏感(S - DD)分离株中检测到唑类抗真菌靶点ERG11基因和外排泵基因(CDR1、CDR2和MDR1)的mRNA水平。在唑类耐药和S - DD分离株中发现了12个编码ERG11中不同氨基酸取代的突变。其中,ERG11基因中的A114S、Y132H和Y257H取代可能主要与唑类耐药有关。综上所述,我们观察到白色念珠菌分离株具有高度的多样性。多种相互关联的潜在机制,包括遗传和环境因素,可能是临床白色念珠菌感染中高表面黏附性或唑类耐药的原因。

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