前往低收入和中等收入国家旅行以及旅行者腹泻会增加尿路感染抗菌治疗不匹配的风险。
Travel to low- and middle-income countries and travellers' diarrhoea increase risk of mismatching antimicrobial therapy for urinary tract infection.
作者信息
Patjas Anu, Kantele Anu
机构信息
Meilahti Vaccine Research Center, MeVac, Department of Infectious Diseases, University of Helsinki and Helsinki University Hospital, FI-00029 HUS Helsinki, Finland.
Human Microbiome Research Unit, University of Helsinki, Haartmaninkatu 3, FI-00290 Helsinki, Finland.
出版信息
J Travel Med. 2025 Apr 25;32(4). doi: 10.1093/jtm/taaf025.
BACKGROUND
Travel to low- and middle-income countries (LMICs) increases the risk of urinary tract infections (UTIs), including those caused by extended-spectrum beta-lactamase-producing Enterobacterales (ESBL-PE). Focusing on international travel, we explored resistance profiles of urinary ESBL-PE and non-ESBL-PE isolates in a low antimicrobial resistance prevalence country and factors associated with UTI treatment failure.
METHODS
During 2015-19, we recruited 18-65-year-old individuals with recent ESBL-PE UTI and a respective cohort of those with non-ESBL-PE UTI to complete questionnaires on symptoms, antibiotic therapies and treatment failure risk factors. We compared uropathogens' resistance profiles amongst patients with or without LMIC travel history and conducted multivariable analyses to identify factors contributing to mismatching antimicrobial treatment (uropathogen resistant to the initial antimicrobial used) and clinical failure.
RESULTS
Amongst non-ESBL-PE UTI patients (n = 187), trimethoprim resistance was more common in isolates from individuals with recent LMIC travel (8/19, 42.1%) compared to those without (30/167, 18.0%) [odds ratio (OR) 3.3, compatibility interval (CI) 95% 1.2-9.0]. ESBL-PE isolates (n = 130) showed no differences in resistance profiles with respect to LMIC travel history.In the group non-ESBL-PE UTI, risk factors included microbiological mismatching recent LMIC travel [adjusted odds ratio (AOR) 3.6, CI 95% 1.0-12.7] and travellers' diarrhoea (AOR 7.1, CI 95% 1.1-45.6); no factors were significantly associated with mismatching in the group ESBL-PE UTI. As risk factors for clinical failure, in the group non-ESBL-PE UTI, we identified microbiological mismatching (AOR 15.2, CI 95% 4.0-57.9), and renal/bladder disease (AOR 5.2, CI 95% 1.1-23.2), and in the group ESBL-PE UTI, microbiological mismatching (AOR 8.1, CI 95% 2.6-24.7).
CONCLUSIONS
LMIC travel increases the risk of nonmatching empiric antimicrobials, concurring with increased trimethoprim resistance rates amongst the non-ESBL-PE isolates. Our data suggest that UTI patients with recent LMIC travel should not be empirically treated with trimethoprim and, when possible, urinary culturing is warranted.
背景
前往低收入和中等收入国家(LMICs)会增加尿路感染(UTIs)的风险,包括由产超广谱β-内酰胺酶肠杆菌科细菌(ESBL-PE)引起的感染。聚焦于国际旅行,我们在一个抗菌药物耐药率较低的国家,探究了泌尿系统ESBL-PE和非ESBL-PE分离株的耐药谱以及与UTI治疗失败相关的因素。
方法
在2015年至2019年期间,我们招募了18至65岁近期患有ESBL-PE UTI的个体以及相应的非ESBL-PE UTI队列,以完成关于症状、抗生素治疗和治疗失败风险因素的问卷调查。我们比较了有或没有LMIC旅行史患者的尿路病原体耐药谱,并进行多变量分析以确定导致抗菌治疗不匹配(尿路病原体对最初使用的抗菌药物耐药)和临床失败的因素。
结果
在非ESBL-PE UTI患者(n = 187)中,与近期无LMIC旅行的个体分离株相比,近期有LMIC旅行的个体分离株中,甲氧苄啶耐药更为常见(8/19,42.1%对比30/167,18.0%)[优势比(OR)3.3,95%相容区间(CI)1.2 - 9.0]。ESBL-PE分离株(n = 130)在耐药谱方面未显示出与LMIC旅行史相关的差异。在非ESBL-PE UTI组中,风险因素包括近期LMIC旅行导致的微生物学不匹配[调整后优势比(AOR)3.6,95%CI 1.0 - 12.7]和旅行者腹泻(AOR 7.1,95%CI 1.1 - 45.6);在ESBL-PE UTI组中,没有因素与不匹配显著相关。作为临床失败的风险因素,在非ESBL-PE UTI组中,我们确定了微生物学不匹配(AOR 15.2,95%CI 4.0 - 57.9)以及肾脏/膀胱疾病(AOR 5.2,95%CI 1.1 - 23.2),在ESBL-PE UTI组中,微生物学不匹配(AOR 8.1,95%CI 2.6 - 24.7)。
结论
前往LMIC旅行会增加经验性抗菌药物不匹配的风险,同时非ESBL-PE分离株中甲氧苄啶耐药率也会增加。我们的数据表明,近期有LMIC旅行的UTI患者不应使用甲氧苄啶进行经验性治疗,并且在可能的情况下,有必要进行尿液培养。
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