Department of Clinical and Chemical Pathology, Faculty of Medicine, Cairo University, 1st Al-Saray Street, Al-Manial, Cairo, 11559, Egypt.
Department of Microbiology and Immunology, Faculty of Pharmacy, Ahram Canadian University, Giza, Egypt.
Eur J Clin Microbiol Infect Dis. 2020 Mar;39(3):583-591. doi: 10.1007/s10096-019-03761-2. Epub 2019 Nov 26.
Neonatal sepsis is a great challenge for clinicians and infection control practitioners, especially in facilities with limited resources. Carbapenem-resistant Klebsiella pneumoniae (CRKP) is rapidly increasing and carriages a major threat to neonates. We aimed to examine phenotypes causing neonatal late onset sepsis (NLOS) in comparison with neonatal early onset sepsis (NEOS) with further investigations of genotypes, and genetic relatedness of CRKP in neonatal late-onset sepsis. Our study included 88 neonates diagnosed with sepsis: 58 with (NLOS) and 30 with (NEOS) from November 2015 to April 2016, at neonatal intensive care unit (NICU) of Cairo University Hospital. K. pneumoniae was the most common encountered pathogen in the NLOS group (37.9%) with a mean sepsis score of 6.39 when compared to the NEOS group (p < 0.05). In Klebsiella group, C-reactive protein and interleukin-6 levels were significantly high (p ˂ 0.001) and 56.5% of the isolates were meropenem resistant. The most prevalent carbapenemase gene was OXA-48 which was identified in 14/23 (60.8%) followed by NDM-1 which was identified in 12/23 (52.2%) as detected by multiplex PCR. Coexistence of both carbapenemases was found in 52.2% (12/23). The bla, bla, and bla genes were not harbored in the isolates. By investigating the genetic relatedness of CRKP by pulsed-field gel electrophoresis, 23 isolates of K. pneumoniae revealed various pulsed-field gel electrophoresis (PFGE) patterns, demonstrating that the isolates were non-clonal. Awareness of the existing phenotypes and genotypes is important for proper treatment and infection control practices.
新生儿败血症是临床医生和感染控制从业者面临的巨大挑战,尤其是在资源有限的医疗机构。耐碳青霉烯类肺炎克雷伯菌(CRKP)的传播迅速增加,对新生儿构成重大威胁。我们旨在研究引起新生儿晚发型败血症(NLOS)的表型与新生儿早发型败血症(NEOS)的表型,并进一步研究 CRKP 基因型及其在新生儿晚发型败血症中的遗传相关性。本研究纳入了 2015 年 11 月至 2016 年 4 月在开罗大学医院新生儿重症监护病房(NICU)诊断为败血症的 88 例新生儿:58 例为 NLOS,30 例为 NEOS。在 NLOS 组中,肺炎克雷伯菌是最常见的病原体(37.9%),其败血症评分平均为 6.39,与 NEOS 组相比(p<0.05)。在克雷伯氏菌组中,C 反应蛋白和白细胞介素 6 水平显著升高(p<0.001),56.5%的分离株对美罗培南耐药。最常见的碳青霉烯酶基因是 OXA-48,在 23 株(60.8%)分离株中检测到,其次是 NDM-1,在 23 株(52.2%)分离株中检测到,这两种基因均通过多重 PCR 检测到。两种碳青霉烯酶同时存在的占 52.2%(12/23)。分离株未携带 blaOXA-48、blaCTX-M 和 blaKPC 基因。通过脉冲场凝胶电泳(PFGE)研究 CRKP 的遗传相关性,23 株肺炎克雷伯菌显示出不同的 PFGE 模式,表明分离株是非克隆的。了解现有的表型和基因型对于正确的治疗和感染控制措施非常重要。
