Analyzing Antibiotic Resistance in Bacteria from Wastewater in Pakistan Using Whole-Genome Sequencing.

IF 4.3 2区 医学 Q1 INFECTIOUS DISEASES Antibiotics-Basel Pub Date : 2024-10-04 DOI:10.3390/antibiotics13100937
Fazal Sattar, Xiao Hu, Anugrah Saxena, Kathy Mou, Huigang Shen, Hazrat Ali, Muhammad Afzal Ghauri, Yasra Sarwar, Aamir Ali, Ganwu Li
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Abstract

Background: Wastewater is a major source of Antibiotic-Resistant Bacteria (ARB) and a hotspot for the exchange of Antibiotic-Resistant Genes (ARGs). The occurrence of Carbapenem-Resistant Bacteria (CRB) in wastewater samples is a major public health concern. Objectives: This study aimed to analyze Antibiotic resistance in bacteria from wastewater sources in Pakistan. Methods: We analyzed 32 bacterial isolates, including 18 Escherichia coli, 4 Klebsiella pneumoniae, and 10 other bacterial isolates using phenotypic antibiotic susceptibility assay and whole-genome sequencing. This study identified the ARGs, plasmid replicons, and integron genes cassettes in the sequenced isolates. One representative isolate was further sequenced using Illumina and Oxford nanopore sequencing technologies. Results: Our findings revealed high resistance to clinically important antibiotics: 91% of isolates were resistant to cefotaxime, 75% to ciprofloxacin, and 62.5% to imipenem, while 31% showed non-susceptibility to gentamicin. All E. coli isolates were resistant to cephalosporins, with 72% also resistant to carbapenems. Sequence analysis showed a diverse resistome, including carbapenamases (blaNDM-5, blaOXA-181), ESBLs (blaCTX-M-15, blaTEM), and AmpC-type β-lactamases (blaCMY). Key point mutations noticed in the isolates were pmrB_Y358N (colistin) and ftsI_N337NYRIN, ftsI_I336IKYRI (carbapenem). The E. coli isolates had 11 different STs, with ST410 predominating (28%). Notably, the E. coli phylogroup A isolate 45EC1, (ST10886) is reported for the first time from wastewater, carrying blaNDM-5, blaCMY-16, and pmrB_Y358N with class 1 integron gene cassette of dfrA12-aadA2-qacEΔ1 on a plasmid-borne contig. Other carbapenamase, blaNDM-1 and blaOXA-72, were detected in K. pneumoniae 22EB1 and Acinetobacter baumannii 51AC1, respectively. The integrons with the gene cassettes encoding antibiotic resistance, and the transport and bacterial mobilization protein, were identified in the sequenced isolates. Ten plasmid replicons were identified, with IncFIB prevalent in 53% of isolates. Combined Illumina and Oxford nanopore sequencing revealed blaNDM-5 on an IncFIA/IncFIC plasmid and is identical to those reported in the USA, Myanmar, and Tanzania. Conclusions: These findings highlight the environmental prevalence of high-risk and WHO-priority pathogens with clinically important ARGs, underscoring the need for a One Health approach to mitigate ARB isolates.

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利用全基因组测序分析巴基斯坦废水中细菌的抗生素耐药性
背景:废水是耐抗生素细菌 (ARB) 的主要来源,也是耐抗生素基因 (ARG) 交流的热点。废水样本中出现耐碳青霉烯类细菌(CRB)是一个重大的公共卫生问题。研究目的本研究旨在分析巴基斯坦废水源细菌的抗生素耐药性。方法我们使用表型抗生素敏感性检测法和全基因组测序法分析了 32 个细菌分离物,包括 18 个大肠埃希菌、4 个肺炎克雷伯菌和 10 个其他细菌分离物。这项研究确定了测序分离物中的 ARGs、质粒复制子和整合子基因盒。利用 Illumina 和牛津纳米孔测序技术对一个代表性分离物进行了进一步测序。结果:我们的研究结果表明,分离物对临床上重要的抗生素具有高度耐药性:91%的分离株对头孢他啶耐药,75%对环丙沙星耐药,62.5%对亚胺培南耐药,31%对庆大霉素不耐药。所有大肠杆菌分离物都对头孢菌素类产生耐药性,72%的分离物还对碳青霉烯类产生耐药性。序列分析表明了耐药性的多样性,包括碳青霉烯酶(blaNDM-5、blaOXA-181)、ESBLs(blaCTX-M-15、blaTEM)和AmpC型β-内酰胺酶(blaCMY)。在分离物中发现的关键点突变是 pmrB_Y358N(可乐定)和 ftsI_N337NYRIN、ftsI_I336IKYRI(碳青霉烯)。大肠杆菌分离物有 11 种不同的 ST,其中以 ST410 为主(28%)。值得注意的是,大肠杆菌 A 系统群分离物 45EC1(ST10886)是首次从废水中检出,它携带 blaNDM-5、blaCMY-16 和 pmrB_Y358N,并在质粒携带的等位基因上带有 dfrA12-aadA2-qacEΔ1 的 1 类整合子基因盒。在肺炎克氏菌 22EB1 和鲍曼不动杆菌 51AC1 中分别检测到了其他碳青霉烯酶 blaNDM-1 和 blaOXA-72。在测序后的分离物中发现了带有编码抗生素耐药性基因盒、转运蛋白和细菌动员蛋白的整合子。鉴定出了 10 个质粒复制子,其中 53% 的分离物普遍存在 IncFIB。结合Illumina和牛津纳米孔测序技术,在IncFIA/IncFIC质粒上发现了blaNDM-5,与美国、缅甸和坦桑尼亚报告的质粒相同。结论这些发现凸显了具有临床重要ARGs的高风险和世卫组织优先病原体在环境中的普遍性,强调了采用 "一体健康 "方法减少ARB分离物的必要性。
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来源期刊
Antibiotics-Basel
Antibiotics-Basel Pharmacology, Toxicology and Pharmaceutics-General Pharmacology, Toxicology and Pharmaceutics
CiteScore
7.30
自引率
14.60%
发文量
1547
审稿时长
11 weeks
期刊介绍: Antibiotics (ISSN 2079-6382) is an open access, peer reviewed journal on all aspects of antibiotics. Antibiotics is a multi-disciplinary journal encompassing the general fields of biochemistry, chemistry, genetics, microbiology and pharmacology. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. Therefore, there is no restriction on the length of papers.
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