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葡萄牙新生儿感染情况(2005 - 2015年):CC17/PI - 2b多重耐药亚谱系的多样化与出现

Causing Neonatal Infections in Portugal (2005-2015): Diversification and Emergence of a CC17/PI-2b Multidrug Resistant Sublineage.

作者信息

Martins Elisabete R, Pedroso-Roussado Cristiano, Melo-Cristino José, Ramirez Mário

机构信息

Faculdade de Medicina, Instituto de Microbiologia, Instituto de Medicina Molecular, Universidade de Lisboa Lisbon, Portugal.

出版信息

Front Microbiol. 2017 Mar 28;8:499. doi: 10.3389/fmicb.2017.00499. eCollection 2017.

Abstract

The molecular characterization of 218 GBS isolates recovered from neonatal invasive infections in Portugal in 2005-2015 revealed the existence of a small number of genetically distinct lineages that were present over a significant time-span. Serotypes III and Ia were dominant in the population, together accounting for >80% of the isolates. Clonal complex 17 included 50% of all isolates, highlighting the importance of the hypervirulent genetic lineage represented by serotype III ST17//PI-1+PI-2b. Serotype Ia was represented mainly by ST23, previously reported as dominant among invasive disease in non-pregnant adults in Portugal, but also by ST24, showing an increased frequency among late-onset disease. Overall erythromycin resistance was 16%, increasing during the study period ( < 0.001). Macrolide resistance was overrepresented among CC1 and CC19 isolates ( < 0.001 and = 0.008, respectively). While representatives of the hypervirulent CC17 lineage were mostly susceptible to macrolides, we identified for the first time in Europe a recently emerging sublineage characterized by the loss of PI-1 (CC17/PI-2b), simultaneously resistant to macrolides, lincosamides, and tetracycline, also exhibiting high-level resistance to streptomycin and kanamycin. The stability and dominance of CC17 among neonatal invasive infections in the past decades indicates that it is extremely well adapted to its niche; however emerging resistance in this genetic background may have significant implications for the prevention and management of GBS disease.

摘要

对2005年至2015年在葡萄牙从新生儿侵袭性感染中分离出的218株B群链球菌(GBS)菌株进行的分子特征分析显示,存在少数在相当长的时间跨度内出现的基因不同的谱系。血清型III和Ia在该群体中占主导地位,两者合计占分离株的80%以上。克隆复合体17包含所有分离株的50%,突出了血清型III ST17//PI-1+PI-2b所代表的高毒力遗传谱系的重要性。血清型Ia主要由ST23代表,此前报道在葡萄牙非妊娠成人的侵袭性疾病中占主导地位,但也由ST24代表,在晚发性疾病中的频率有所增加。总体红霉素耐药率为16%,在研究期间有所上升(P<0.001)。大环内酯类耐药在CC1和CC19分离株中占比过高(分别为P<0.001和P = 0.008)。虽然高毒力CC17谱系的代表大多对大环内酯类敏感,但我们在欧洲首次鉴定出一个最近出现的亚谱系,其特征是PI-1缺失(CC17/PI-2b),同时对大环内酯类、林可酰胺类和四环素耐药,对链霉素和卡那霉素也表现出高水平耐药。在过去几十年中,CC17在新生儿侵袭性感染中的稳定性和主导地位表明它非常适应其生态位;然而,在这种遗传背景下出现的耐药性可能对GBS疾病的预防和管理产生重大影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bc5/5368217/b5d24215552d/fmicb-08-00499-g0001.jpg

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