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肠道菌群特征可预测尿路感染的18个月发病概率及抗菌药物敏感性。

Gut resident profile predicts the eighteen-month probability and antimicrobial susceptibility of urinary tract infections.

作者信息

Tchesnokova Veronika, Larson Lydia, Basova Irina, Sledneva Yulia, Choudhury Debarati, Solyanik Thalia, Heng Jennifer, Bonilla Teresa Cristina, Pasumansky Isaac, Bowers Victoria, Pham Sophia, Madziwa Lawrence T, Holden Erika, Tartof Sara Y, Ralston James D, Sokurenko Evgeni V

机构信息

Department of Microbiology, University of Washington School of Medicine, 1705 NE Pacific St., Seattle, WA 98195, USA.

Kaiser Permanente Washington, 2715 Naches Ave. SW, Renton, WA 98057, USA.

出版信息

medRxiv. 2024 Apr 9:2024.04.05.24305377. doi: 10.1101/2024.04.05.24305377.

Abstract

BACKGROUND

Community-acquired UTI is the most common bacterial infection managed in general medical practice that can lead to life-threatening outcomes. While UTIs are primarily caused by colonizing the patient's gut, it is unclear whether the gut resident profiles can predict the person's risks for UTI and optimal antimicrobial treatments. Thus, we conducted an eighteen-month long community-based observational study of fecal colonization and UTI in women aged 50 years and above.

METHODS AND FINDINGS

We enrolled a total of 1,804 women distributed among age groups 50-59 yo (437 participants), 60-69 yo (632), 70-79 yo (532), and above 80 yo (203), lacking antibiotic prescriptions for at least one year. The provided fecal samples were plated for the presence of and other enterobacteria resistant to trimethoprim/sulfamethoxazole (TMP/STX), ciprofloxacin (CIP) and 3 generation cephalosporins (3GC). was also characterized as belonging to the pandemic multi-drug resistant clonal groups ST131 (subclone H30) and ST1193. Following sample collection, the women were monitored for 18 months for occurrence of UTI. was cultured from 90.8% fecal samples, with 24.1% containing bacteria resistant to TMP/STX, 19.4% to CIP, and 7.9% to 3GC. In 62.5% samples, only all-susceptible were present. Overall, there were no age-related differences in resistance prevalence. However, while the total H30 and ST1193 carriage rates were similar (4.3% and 4.2%, respectively), there was a notable increase of H30 carriage with age (P = .001), while carriage decreased with age for ST1193 (P = .057).Within 18 months, 184 women (10.2%) experienced at least one episode of UTI - 10.9% among the gut carriers and 3.0% among the non-carriers (P=.0013). The UTI risk among carriers of H30 but not ST1193 was significantly above average (24.3%, P = .0004). The UTI probability increased with age, occurring in 6.4% of 50-59 yo and 19.7% of 80+ yo (P<.001), with the latter group being especially at high risk for UTI, if they were colonized by H30 (40.0%, P<.001). was identified in 88.1% of urine samples, with 16.1% resistant to TMP/STX, 16.1% to CIP, 4.2% to 3GC and 73.1% to none of the antibiotics. Among tested urinary resistant to antibiotics, 86.1% matched the resistance profile of in the fecal samples, with the clonotyping and whole genome sequencing confirming the matching strains' identity. Positive predictive value (PPV) of using gut resistance profiles to predict UTI pathogens' susceptibility to TMP/STX, CIP, 3GC and all three antibiotics were 98.4%, 98.3%, 96.6% and 95.3%, respectively. Corresponding negative predictive values (NPV) were 63.0%, 54.8%, 44.4% and 75.8%, respectively. The AUC ROC curve values for the accuracy of fecal diagnostic testing for the prediction of UTI resistance ranged .86-.89. The fecal test-guided drug-bug mismatch rate for empirical (pre-culture) prescription of TMP-SXT or CIP is reduced to ≤2% in 89.6% of patients and 94.8% of patients with an optional 3GC prescription.

CONCLUSION

The resistance profile and clonal identity of gut colonizing , along with the carrier's age, can inform personalized prediction of a patients' UTI risk and the UTI pathogen's antibiotic susceptibility within an 18-month period.

摘要

背景

社区获得性尿路感染是普通医疗实践中最常见的细菌感染,可能导致危及生命的后果。虽然尿路感染主要是由患者肠道定植引起的,但尚不清楚肠道菌群特征是否可以预测个体发生尿路感染的风险以及最佳抗菌治疗方案。因此,我们对50岁及以上女性进行了一项为期18个月的基于社区的粪便定植与尿路感染观察性研究。

方法与结果

我们共纳入了1804名女性,分布在50 - 59岁(437名参与者)、60 - 69岁(632名)、70 - 79岁(532名)和80岁以上(203名)年龄组,且至少一年未使用抗生素。对提供的粪便样本进行平板接种,以检测是否存在对甲氧苄啶/磺胺甲恶唑(TMP/STX)、环丙沙星(CIP)和第三代头孢菌素(3GC)耐药的大肠杆菌及其他肠杆菌。大肠杆菌还被鉴定为属于大流行的多重耐药克隆群ST131(亚克隆H30)和ST1193。样本采集后,对这些女性进行了18个月的尿路感染发生情况监测。90.8%的粪便样本培养出大肠杆菌,其中24.1%含有对TMP/STX耐药的细菌,19.4%对CIP耐药,7.9%对3GC耐药。在62.5%的样本中,仅存在全敏感的大肠杆菌。总体而言,耐药率在各年龄组之间无差异。然而,虽然H30和ST1193的总体携带率相似(分别为4.3%和4.2%),但H30的携带率随年龄显著增加(P = 0.001),而ST1193的携带率随年龄下降(P = 0.057)。在18个月内,184名女性(10.2%)经历了至少一次尿路感染——肠道大肠杆菌携带者中为10.9%,非携带者中为3.0%(P = 0.0013)。H30但非ST1193携带者的尿路感染风险显著高于平均水平(24.3%,P = 0.0004)。尿路感染概率随年龄增加,50 - 59岁女性中为6.4%,80岁及以上女性中为19.7%(P < 0.001),如果80岁及以上女性被H30定植,其尿路感染风险尤其高(40.0%,P < 0.001)。88.1%的尿液样本中检测出大肠杆菌,其中16.1%对TMP/STX耐药,16.1%对CIP耐药,4.2%对3GC耐药,73.1%对所有抗生素均不耐药。在检测出对抗生素耐药的尿液大肠杆菌中,86.1%与粪便样本中大肠杆菌的耐药谱相匹配,克隆分型和全基因组测序证实了匹配菌株的同一性。利用肠道耐药谱预测尿路感染病原体对TMP/STX、CIP、3GC及所有三种抗生素敏感性的阳性预测值(PPV)分别为98.4%、98.3%、96.6%和95.3%。相应的阴性预测值(NPV)分别为63.0%、54.8%、44.4%和75.8%。粪便诊断检测预测尿路感染耐药性准确性的AUC ROC曲线值在0.86 - 0.89之间。在89.6%的患者中,以及在94.8%接受可选3GC处方的患者中,TMP - SXT或CIP经验性(培养前)处方的粪便检测引导的药物 - 细菌不匹配率降至≤2%。

结论

肠道定植大肠杆菌的耐药谱和克隆特征,以及携带者的年龄,可在18个月内为个性化预测患者的尿路感染风险及尿路感染病原体的抗生素敏感性提供依据。

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