Comprehensive genomics reveals novel sequence types of multidrug resistant Klebsiella oxytoca with uncharacterized capsular polysaccharide K- and lipopolysaccharide O-antigen loci from the National Hospital of Uganda

IF 2.6 4区医学 Q3 INFECTIOUS DISEASES

Infection Genetics and Evolution Pub Date : 2024-07-11 DOI:10.1016/j.meegid.2024.105640

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Abstract

The Klebsiella oxytoca complex comprises diverse opportunistic bacterial pathogens associated with hospital and community-acquired infections with growing alarming antimicrobial resistance. We aimed to uncover the genomic features underlying the virulence and antimicrobial resistance of isolates from Mulago National Hospital in Uganda. We coupled whole genome sequencing with Pathogenwatch multilocus sequence typing (MLST) and downstream bioinformatic analysis to delineate sequence types (STs) capsular polysaccharide K- and O-antigen loci, along with antimicrobial resistance (AMR) profiles of eight clinical isolates from the National Referral Hospital of Uganda. Our findings revealed that only two isolates (RSM6774 and RSM7756) possess a known capsular polysaccharide K-locus (KL74). The rest carry various unknown K-loci (KL115, KL128, KLI52, KL161 and KLI63). We also found that two isolates possess unknown loci for the lipopolysaccharide O-antigen (O1/O2v1 type OL104 and unknown O1). The rest possess known O1 and O3 serotypes. From MLST, we found four novel sequence types (STs), carrying novel alleles for the housekeeping genes glyceraldehyde-6-phosphate dehydrogenase A (gapA), glucose-6-phosphate isomerase (pgi), and RNA polymerase subunit beta (rpoB). Our AMR analysis revealed that all the isolates are resistant to ampicillin and ceftriaxone, with varied resistance to other antibiotics, but all carry genes for extended-spectrum beta-lactamases (ESBLs). Notably, one strain (RSM7756) possesses outstanding chromosomal and plasmid-encoded AMR to beta-lactams, cephalosporins, fluoroquinolones and methoprims. Conclusively, clinical samples from Mulago National Referral Hospital harbor novel STs and multidrug resistant K. oxytoca strains, with significant public health importance, which could have been underrated.

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综合基因组学揭示了乌干达国立医院中具有未定性胶囊多糖和 O 抗原位点的新型耐多药氧雷伯氏菌序列类型。

氧合克雷伯氏菌复合体由多种机会性细菌病原体组成，与医院和社区获得性感染有关，其抗菌药耐药性日益惊人。我们的目的是揭示乌干达穆拉戈国立医院分离菌毒力和抗菌药耐药性的基因组特征。我们将全基因组测序与病原观察多焦点序列分型（MLST）和下游生物信息学分析相结合，对来自乌干达国家转诊医院的 8 株临床分离株的荚膜多糖 K-和 O-抗原位点的序列类型（ST）以及抗菌药耐药性（AMR）谱进行了划分。我们的研究结果表明，只有两个分离株（RSM6774 和 RSM7756）具有已知的荚膜多糖 K-位点（KL74）。其余的分离物带有各种未知的 K-位点（KL115、KL128、KLI52、KL161 和 KLI63）。我们还发现，两个分离物具有未知的脂多糖 O 抗原位点（O1/O2v1 型 OL104 和未知 O1）。其余的则具有已知的 O1 和 O3 血清型。通过 MLST，我们发现了四种新型序列类型（STs），它们携带有管理基因甘油醛-6-磷酸脱氢酶 A（gapA）、葡萄糖-6-磷酸异构酶（pgi）和 RNA 聚合酶亚基 beta（rpoB）的新型等位基因。我们的 AMR 分析表明，所有分离株都对氨苄西林和头孢曲松具有耐药性，对其他抗生素的耐药性也不尽相同，但都携带广谱β-内酰胺酶（ESBLs）基因。值得注意的是，其中一株菌株（RSM7756）对β-内酰胺类、头孢菌素类、氟喹诺酮类和甲氧苄啶类具有出色的染色体和质粒编码 AMR。总之，穆拉戈国家转诊医院的临床样本中存在新型STs和耐多药氧雷杆菌菌株，对公共卫生具有重要意义，而这一点可能被低估了。

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来源期刊

Infection Genetics and Evolution 医学-传染病学

CiteScore

8.40

自引率

0.00%

发文量

215

审稿时长

82 days

期刊介绍： (aka Journal of Molecular Epidemiology and Evolutionary Genetics of Infectious Diseases -- MEEGID) Infectious diseases constitute one of the main challenges to medical science in the coming century. The impressive development of molecular megatechnologies and of bioinformatics have greatly increased our knowledge of the evolution, transmission and pathogenicity of infectious diseases. Research has shown that host susceptibility to many infectious diseases has a genetic basis. Furthermore, much is now known on the molecular epidemiology, evolution and virulence of pathogenic agents, as well as their resistance to drugs, vaccines, and antibiotics. Equally, research on the genetics of disease vectors has greatly improved our understanding of their systematics, has increased our capacity to identify target populations for control or intervention, and has provided detailed information on the mechanisms of insecticide resistance. However, the genetics and evolutionary biology of hosts, pathogens and vectors have tended to develop as three separate fields of research. This artificial compartmentalisation is of concern due to our growing appreciation of the strong co-evolutionary interactions among hosts, pathogens and vectors. Infection, Genetics and Evolution and its companion congress [MEEGID](http://www.meegidconference.com/) (for Molecular Epidemiology and Evolutionary Genetics of Infectious Diseases) are the main forum acting for the cross-fertilization between evolutionary science and biomedical research on infectious diseases. Infection, Genetics and Evolution is the only journal that welcomes articles dealing with the genetics and evolutionary biology of hosts, pathogens and vectors, and coevolution processes among them in relation to infection and disease manifestation. All infectious models enter the scope of the journal, including pathogens of humans, animals and plants, either parasites, fungi, bacteria, viruses or prions. The journal welcomes articles dealing with genetics, population genetics, genomics, postgenomics, gene expression, evolutionary biology, population dynamics, mathematical modeling and bioinformatics. We also provide many author benefits, such as free PDFs, a liberal copyright policy, special discounts on Elsevier publications and much more. Please click here for more information on our author services .