[Investigation of sasX, ACME and Various Virulence Factors in Coagulase Negative Staphylococcal Strains Identified as Bloodstream Infection Agents and Contamination].

IF 1.1 4区 医学 Q4 MICROBIOLOGY Mikrobiyoloji bulteni Pub Date : 2024-10-01 DOI:10.5578/mb.20249678
Büşra Dönmez, Melek Demir
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Abstract

The aim of this study was to investigate the frequency of sasX, arginine catabolic mobile element (ACME) genes, biofilm formation and some biofilm related virulence factor genes in causative and contaminant coagulase negative staphylococci (CNS) strains isolated from blood cultures. Of the 150 CNS strains included in the study, 50 were grouped as infectious agents and 100 as contaminants. Biofilm formation of the strains was investigated by microplate method and the presence of sasX, ACME, mecA and biofilm associated virulence factor genes icaA, icaD, aap, bhp and IS256 were investigated by inhouse polymerase chain reaction method. While 52% of the strains in the infectious agents group and 57% of the strains in the contamination group phenotypically formed biofilm; when the levels of biofilm positivity were compared, it was observed that the strains in the infectious agents group (30%) formed biofilm at a stronger level than the strains in the contamination group (14%) (p= 0.027). Biofilm-associated icaA, icaD, IS256, aap and bhp genes were found positive in 33%, 45%, 43%, 74% and 6% of the strains in the contamination group and 64%, 62%, 64%, 74% and 8% of the strains in the infectious agents group, respectively. ACME gene regions arcA, kdpA and opp3B and sasX related gene region were found positive in 30%, 7%, 8% and 14% of the strains in the contamination group and in 12%, 2%, 6% and 10% of the strains in the infectious agents group, respectively. The positivity of icaA, icaD and IS256 genes alone or together in the infectious agents group (p< 0.001, p= 0.050, p= 0.015, respectively) and the positivity of ACME and arcA in the contamination group (p= 0.008, p= 0.015, respectively) were statistically significantly higher. No significant difference was found between the two groups for sasX, aap and bhp genes. In conclusion, among the CNS strains isolated from blood cultures, strains that form a strong biofilm and are positive for biofilm-associated gene regions alone or together can be considered as infectious agents, while strains that are found to be arcA positive in the absence of clinical signs of infection can be considered as contaminants.

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[凝固酶阴性葡萄球菌中sasX、ACME及多种毒力因子的研究]。
本研究的目的是研究从血液培养中分离的致病性和污染物凝固酶阴性葡萄球菌(CNS)菌株中sasX、精氨酸分解代谢移动元件(ACME)基因、生物膜形成和一些生物膜相关毒力因子基因的频率。在研究中包括的150种中枢神经系统菌株中,50种被归为感染原,100种被归为污染物。采用微孔板法检测菌株的生物膜形成情况,采用室内聚合酶链反应法检测sasX、ACME、mecA及生物膜相关毒力因子基因icaA、icaD、aap、bhp和IS256的表达情况。感染原组中52%的菌株和污染组中57%的菌株表型形成生物膜;在比较生物膜阳性水平时,发现感染原组(30%)的菌株形成的生物膜水平高于污染组(14%)(p= 0.027)。污染组生物膜相关icaA、icaD、IS256、aap和bhp基因阳性比例分别为33%、45%、43%、74%和6%,感染原组生物膜相关icaA、icaD、IS256、aap和bhp基因阳性比例分别为64%、62%、64%、74%和8%。ACME基因区arcA、kdpA、opp3B和sasX相关基因区在污染组中分别为30%、7%、8%和14%,在感染原组中分别为12%、2%、6%和10%。感染原组icaA、icaD、IS256基因单独或共同阳性率(p< 0.001, p= 0.050, p= 0.015)和污染组ACME、arcA基因阳性率(p= 0.008, p= 0.015)均显著高于感染原组。sasX、aap和bhp基因在两组间无显著差异。综上所述,在血液培养分离的CNS菌株中,形成强生物膜且生物膜相关基因区单独或共同呈阳性的菌株可视为感染原,而在没有临床感染体征的情况下发现arcA阳性的菌株可视为污染物。
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来源期刊
Mikrobiyoloji bulteni
Mikrobiyoloji bulteni 生物-微生物学
CiteScore
1.60
自引率
20.00%
发文量
50
审稿时长
6-12 weeks
期刊介绍: Bulletin of Microbiology is the scientific official publication of Ankara Microbiology Society. It is published quarterly in January, April, July and October. The aim of Bulletin of Microbiology is to publish high quality scientific research articles on the subjects of medical and clinical microbiology. In addition, review articles, short communications and reports, case reports, editorials, letters to editor and other training-oriented scientific materials are also accepted. Publishing language is Turkish with a comprehensive English abstract. The editorial policy of the journal is based on independent, unbiased, and double-blinded peer-review. Specialists of medical and/or clinical microbiology, infectious disease and public health, and clinicians and researchers who are training and interesting with those subjects, are the target groups of Bulletin of Microbiology.
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