Emergence of extensive drug resistance and high prevalence of multidrug resistance among clinical Proteus mirabilis isolates in Egypt.

IF 4.6 2区 医学 Q1 MICROBIOLOGY Annals of Clinical Microbiology and Antimicrobials Pub Date : 2024-05-24 DOI:10.1186/s12941-024-00705-3
Maggi ElTaweel, Heba Shehta Said, Rasha Barwa
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Abstract

Background: Proteus mirabilis is an opportunistic pathogen that has been held responsible for numerous nosocomial and community-acquired infections which are difficult to be controlled because of its diverse antimicrobial resistance mechanisms.

Methods: Antimicrobial susceptibility patterns of P. mirabilis isolates collected from different clinical sources in Mansoura University Hospitals, Egypt was determined. Moreover, the underlying resistance mechanisms and genetic relatedness between isolates were investigated.

Results: Antimicrobial susceptibility testing indicated elevated levels of resistance to different classes of antimicrobials among the tested P. mirabilis clinical isolates (n = 66). ERIC-PCR showed great diversity among the tested isolates. Six isolates (9.1%) were XDR while all the remaining isolates were MDR. ESBLs and AmpCs were detected in 57.6% and 21.2% of the isolates, respectively, where blaTEM, blaSHV, blaCTX-M, blaCIT-M and blaAmpC were detected. Carbapenemases and MBLs were detected in 10.6 and 9.1% of the isolates, respectively, where blaOXA-48 and blaNDM-1 genes were detected. Quinolone resistant isolates (75.8%) harbored acc(6')-Ib-cr, qnrD, qnrA, and qnrS genes. Resistance to aminoglycosides, trimethoprim-sulfamethoxazole and chloramphenicol exceeded 80%. Fosfomycin was the most active drug against the tested isolates as only 22.7% were resistant. Class I or II integrons were detected in 86.4% of the isolates. Among class I integron positive isolates, four different gene cassette arrays (dfrA17- aadA5, aadB-aadA2, aadA2-lnuF, and dfrA14-arr-3-blaOXA-10-aadA15) and two gene cassettes (dfrA7 and aadA1) were detected. While class II integron positive isolates carried four different gene cassette arrays (dfrA1-sat1-aadA1, estXVr-sat2-aadA1, lnuF- dfrA1-aadA1, and dfrA1-sat2).

Conclusion: P. Mirabilis ability to acquire resistance determinants via integrons may be held responsible for the elevated rates of antimicrobial resistance and emergence of XDR or even PDR strains limiting the available therapeutic options for management of infections caused by those strains.

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埃及奇异变形杆菌临床分离株中出现广泛耐药性和多重耐药性的高流行率。
背景:mirabilis 变形杆菌是一种机会性病原体,是众多医院内感染和社区获得性感染的罪魁祸首,由于其具有多种抗菌药耐药机制而难以控制:方法:对从埃及曼苏拉大学医院不同临床来源采集的P. mirabilis分离株的抗菌药敏感性模式进行了测定。此外,还调查了分离株之间的潜在耐药机制和遗传相关性:结果:抗菌药敏感性测试表明,受测的奇异变形杆菌临床分离株(n = 66)对不同类别抗菌药的耐药性水平较高。ERIC-PCR显示受测分离株之间存在很大的多样性。有 6 个分离株(9.1%)具有 XDR,而其余所有分离株都具有 MDR。分别有 57.6% 和 21.2% 的分离物检测到 ESBLs 和 AmpCs,其中检测到 blaTEM、blaSHV、blaCTX-M、blaCIT-M 和 blaAmpC。在检测到 blaOXA-48 和 blaNDM-1 基因的分离物中,分别有 10.6% 和 9.1% 检测到碳青霉烯酶和 MBL。喹诺酮耐药分离物(75.8%)携带 acc(6')-Ib-cr、qnrD、qnrA 和 qnrS 基因。对氨基糖苷类、三甲双氨-磺胺甲噁唑和氯霉素的耐药性超过 80%。磷霉素是对测试分离株最有效的药物,只有 22.7% 的分离株对其产生耐药性。在 86.4% 的分离株中检测到了 I 类或 II 类整合子。在 I 类整合素阳性的分离物中,检测到了四个不同的基因盒阵列(dfrA17- aadA5、aadB-aadA2、aadA2-lnuF 和 dfrA14-arr-3-blaOXA-10-aadA15)和两个基因盒(dfrA7 和 aadA1)。而 II 类整合素阳性分离物携带有 4 个不同的基因盒阵列(dfrA1-sat1-aadA1、estXVr-sat2-aadA1、lnuF- dfrA1-aadA1 和 dfrA1-sat2):结论:P. Mirabilis通过整合子获得抗药性决定因子的能力可能是抗菌药耐药率升高和XDR甚至PDR菌株出现的原因,这限制了治疗由这些菌株引起的感染的可用疗法。
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来源期刊
CiteScore
8.60
自引率
0.00%
发文量
49
审稿时长
>12 weeks
期刊介绍: Annals of Clinical Microbiology and Antimicrobials considers good quality, novel and international research of more than regional relevance. Research must include epidemiological and/or clinical information about isolates, and the journal covers the clinical microbiology of bacteria, viruses and fungi, as well as antimicrobial treatment of infectious diseases. Annals of Clinical Microbiology and Antimicrobials is an open access, peer-reviewed journal focusing on information concerning clinical microbiology, infectious diseases and antimicrobials. The management of infectious disease is dependent on correct diagnosis and appropriate antimicrobial treatment, and with this in mind, the journal aims to improve the communication between laboratory and clinical science in the field of clinical microbiology and antimicrobial treatment. Furthermore, the journal has no restrictions on space or access; this ensures that the journal can reach the widest possible audience.
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