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2019 年至 2021 年间,中国中部一家三级综合性教学医院基于全基因组序列,发现 4 株同时携带 bla 和 bla 的碳青霉烯类耐药肺炎克雷伯菌的耐药性和毒力特征。

Antibiotic resistance and virulence characteristics of four carbapenem-resistant Klebsiella pneumoniae strains coharbouring bla and bla based on whole genome sequences from a tertiary general teaching hospital in central China between 2019 and 2021.

机构信息

Department of Pharmacy, School of Pharmacy, Shanxi Medical University, Taiyuan, Shanxi, PR China; Shanxi Jinzhong Health School, Jinzhong, Shanxi, PR China.

Department of Pharmacy, School of Pharmacy, Shanxi Medical University, Taiyuan, Shanxi, PR China.

出版信息

Microb Pathog. 2023 Feb;175:105969. doi: 10.1016/j.micpath.2023.105969. Epub 2023 Jan 4.

Abstract

OBJECTIVE

Carbapenem-resistant Klebsiella pneumoniae (CRKP) infection is a worldwide health issue that poses a serious threat to public health. This study summarizes the clinical features of four patients with CRKP coproducing NDM and KPC infections and further analyses the molecular typing, resistance and virulence factors of the four CRKP strains.

METHODS

Of the twenty-two CRKP isolates, four strains coharbouring bla and bla isolated from four patients were screened by Sanger sequencing between October 2019 and April 2021. Demographics, clinical and pathological data of the four patients were collected through electronic medical records. Antimicrobial susceptibility testing, biofilm formation assays and serum bactericidal assays were performed on the four isolates. The antibiotic resistance and virulence genes were investigated by whole-genome sequencing. Sequence types (STs) were determined by multilocus sequence typing, and serotypes were identified by wzi gene sequencing.

RESULTS

Three patients recovered, and one patient stopped treatment. Four strains were multiple carbapenemase producers: KPC-2, NDM-4, SME-5 and IMI-4 coproducer; KPC-2, NDM-1 and SME-3 coproducer; KPC-2, NDM-1 and IMI-3 coproducer; KPC-2 and NDM-5 coproducer. They also harboured ESBL genes and mutations in the efflux pump regulator genes. They were multidrug resistant but sensitive to tigecycline and colistin. Four isolates had moderate biofilm-forming abilities and carried various virulence genes, including siderophores, type 1 fimbriae and E. coli common pilus. Only the NO. 3 strain was resistant to the serum. The STs and serotypes of the four strains were ST11 and KL64, ST337 and none, ST307 and KL102KL149KL155, and ST29 and K54, respectively.

CONCLUSION

Four CRKP strains coharbouring bla and bla also carried other carbapenemase genes. Notably, the NO. 1 isolate carrying four carbapenemase genes has not been reported globally until now. Four strains exhibited a high level of resistance to multiple antibiotics. Additionally, three of the four patients were exposed to invasive medical devices that provided an environment for biofilm formation. Meanwhile, three strains with adhesion genes as moderate biofilm formers might form biofilms resulting in long hospital stays, increasing therapeutic difficulty, and even treatment failure. This study reminds clinicians that CRKP strains with multiple carbapenemase genes emerged in our hospital, and stronger measures should be taken to the control of nosocomial infections.

摘要

目的

耐碳青霉烯类肺炎克雷伯菌(CRKP)感染是一个全球性的健康问题,对公共卫生构成严重威胁。本研究总结了 4 例同时产 NDM 和 KPC 型碳青霉烯酶 CRKP 感染患者的临床特征,并进一步分析了 4 株 CRKP 株的分子分型、耐药性和毒力因子。

方法

对 2019 年 10 月至 2021 年 4 月期间通过 Sanger 测序筛选出的 22 株 CRKP 分离株中,4 株同时携带 bla 和 bla 的菌株进行了研究。通过电子病历收集了 4 名患者的人口统计学、临床和病理数据。对 4 株分离株进行了药敏试验、生物膜形成试验和血清杀菌试验。通过全基因组测序检测抗生素耐药基因和毒力基因。通过多位点序列分型(MLST)确定序列型(ST),通过 wzi 基因测序确定血清型。

结果

3 例患者痊愈,1 例患者停止治疗。4 株菌均为多种碳青霉烯酶产生菌:KPC-2、NDM-4、SME-5 和 IMI-4 共同产生;KPC-2、NDM-1 和 SME-3 共同产生;KPC-2、NDM-1 和 IMI-3 共同产生;KPC-2 和 NDM-5 共同产生。它们还携带 ESBL 基因和外排泵调节基因的突变。它们对多种药物耐药,但对替加环素和黏菌素敏感。4 株菌均具有中等的生物膜形成能力,并携带各种毒力基因,包括铁载体、I 型菌毛和大肠普通菌毛。只有 3 号菌株对血清有耐药性。4 株菌的 ST 和血清型分别为 ST11 和 KL64、ST337 和无、ST307 和 KL102KL149KL155、ST29 和 K54。

结论

4 株同时携带 bla 和 bla 的 CRKP 株还携带其他碳青霉烯酶基因。值得注意的是,目前全球尚未报道携带 4 种碳青霉烯酶基因的 1 号分离株。4 株菌对多种抗生素均表现出高水平耐药。此外,3 例患者均接触过侵入性医疗器械,为生物膜形成提供了环境。同时,3 株具有中度生物膜形成能力的黏附基因菌株可能会形成生物膜,导致住院时间延长,增加治疗难度,甚至治疗失败。本研究提醒临床医生,我院出现了同时携带多种碳青霉烯酶基因的 CRKP 菌株,应采取更强有力的措施控制医院感染。

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