尼泊尔特里布万大学教学医院肾脏疾病患者尿路病原体的抗菌素耐药性和生物膜生成

IF 2.1 4区医学 Q3 PHARMACOLOGY & PHARMACY

Journal of Clinical Pharmacy and Therapeutics Pub Date : 2023-07-19 DOI:10.1155/2023/4867817

A. Dahal, K. Shrestha, R. Karki, Saraswati Bhattarai, Shiva Aryal, S. Deo, B. Regmi, M. Willcox, S. K. Mishra

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引用次数: 0

摘要

背景。各种抗生素是由医生的经验，以应付肾脏疾病患者的感染。尿路感染(UTI)通常是由形成生物膜的多药耐药(MDR)尿路病原体引起的。本研究旨在分析肾脏疾病患者尿路感染菌株的抗生素谱及这些菌株的生物膜形成能力。方法:2017年8月至2018年1月，102名临床诊断为尿路感染和肾脏疾病的患者被纳入研究。按照标准方法处理干净的中游尿液样本以分离和鉴定细菌。106株分离菌的抗生素谱采用Kirby-Bauer圆盘扩散法。在组织培养板中检测生物膜的形成。结果。尿路感染在肾脏疾病中的发病率为19.1%。多数患者诊断为慢性肾病(18.63%)、肾病综合征(16.67%)和肾结石(14.71%)。最常见的泌尿系病原菌为大肠杆菌(52.8%)、肺炎克雷伯菌(16%)和肠球菌(15.0%)。头孢曲松是最常用的经验处方抗生素(37%)，而呋喃妥因是最常用的调整治疗抗生素(36.1%)。在一线和二线抗生素中，革兰氏阴性菌对阿米卡星(70.7%)、美罗培南(70.7%)、头孢哌酮-舒巴坦(70.0%)、哌拉西林-他唑巴坦(67.2%)、庆大霉素(66.7%)和呋喃妥英硝基(66.7%)最为敏感。革兰氏阳性菌对强力霉素(90.0%)、呋喃妥英(72.2%)、庆大霉素(66.7%)和四环素(62.5%)敏感。所有MDR革兰氏阴性尿路病原菌均对硫酸粘菌素和多粘菌素b敏感。106株分离菌中，74.5%产生生物膜，70.8%为MDR。67.0%的病例(包括耐多药和产膜细菌)需要调整经验性治疗。结论。氨基糖苷类、碳青霉烯类、β -内酰胺类抑制剂、硝基呋喃类抗生素可能是治疗住院肾病患者尿路病原菌的最佳一线经验疗法。必须定期监测耐药性模式和研究尿路病原体的生物膜形成，以确保对患者的有效管理。

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Antimicrobial Resistance and Biofilm Production in Uropathogens from Renal Disease Patients Admitted to Tribhuvan University Teaching Hospital, Nepal

Background. Various antibiotics are prescribed empirically by physicians to cope with infections in renal disease patients. A urinary tract infection (UTI) is often caused by biofilm-forming multidrug-resistant (MDR) uropathogens. This study aimed to analyze the antibiogram of UTI strains from renal disease patients and the biofilm-forming ability of those strains. Methods. 102 patients clinically diagnosed with a UTI and renal disease were recruited into the study from August 2017 to January 2018. Clean-catch midstream urine samples were processed for the isolation and identification of the bacteria following standard methodologies. The antibiogram of the isolates (n = 106) was produced by the Kirby–Bauer disc diffusion method. Detection of biofilm formation was performed in tissue culture plates. Results. The incidence of a UTI in renal disease was 19.1%. Most patients were diagnosed with chronic kidney disease (18.63%), nephrotic syndrome (16.67%), and nephrolithiasis (14.71%). The commonest uropathogens were Escherichia coli (52.8%), Klebsiella pneumoniae (16%), and Enterococcus spp. (15.0%). Ceftriaxone was the most common antibiotic prescribed empirically (37%), whereas nitrofurantoin was the most prescribed antibiotic as adjusted therapy (36.1%). Among the first- and second-line antibiotics, most Gram-negative bacteria were sensitive to amikacin (70.7%), meropenem (70.7%), cefoperazone-sulbactam (70.0%), piperacillin-tazobactam (67.2%), gentamicin (66.7%), and nitrofurantoin (66.7%). Most Gram-positive bacteria were sensitive to doxycycline (90.0%), nitrofurantoin (72.2%), gentamicin (66.7%), and tetracycline (62.5%). All MDR Gram-negative uropathogens were susceptible to colistin sulfate and polymyxin B. Among the 106 isolates, 74.5% produced biofilms and 70.8% were MDR. In 67.0% of cases, including both MDR and biofilm-producing bacteria, the empirical therapy needed adjustment. Conclusions. Aminoglycoside, carbapenem, beta-lactam inhibitor, and nitrofuran group of antibiotics may be the optimal first-line empirical therapies for uropathogens in hospitalized renal disease patients. Regular surveillance of resistance patterns and the study of biofilm formation in uropathogens must be performed to ensure effective management of the patients.

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来源期刊

Journal of Clinical Pharmacy and Therapeutics 医学-药学

CiteScore

4.10

自引率

5.00%

发文量

226

审稿时长

6 months

期刊介绍： The Journal of Clinical Pharmacy and Therapeutics provides a forum for clinicians, pharmacists and pharmacologists to explore and report on issues of common interest. Reports and commentaries on current issues in medical and pharmaceutical practice are encouraged. Papers on evidence-based clinical practice and multidisciplinary collaborative work are particularly welcome. Regular sections in the journal include: editorials, commentaries, reviews (including systematic overviews and meta-analyses), original research and reports, and book reviews. Its scope embraces all aspects of clinical drug development and therapeutics, including: Rational therapeutics Evidence-based practice Safety, cost-effectiveness and clinical efficacy of drugs Drug interactions Clinical impact of drug formulations Pharmacogenetics Personalised, stratified and translational medicine Clinical pharmacokinetics.