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医院抗菌药物管理:新冠病毒感染及抗生素暴露后口腔微生物群特征分析

Hospital antimicrobial stewardship: profiling the oral microbiome after exposure to COVID-19 and antibiotics.

作者信息

Buendia Patricia, Fernandez Krystal, Raley Castle, Rahnavard Ali, Crandall Keith A, Castro Jose Guillermo

机构信息

Lifetime Omics, Miami, FL, United States.

The George Washington University Genomics Core, Milken Institute School of Public Health, The George Washington University, Washington, DC, United States.

出版信息

Front Microbiol. 2024 Feb 27;15:1346762. doi: 10.3389/fmicb.2024.1346762. eCollection 2024.

Abstract

INTRODUCTION

During the COVID-19 Delta variant surge, the CLAIRE cross-sectional study sampled saliva from 120 hospitalized patients, 116 of whom had a positive COVID-19 PCR test. Patients received antibiotics upon admission due to possible secondary bacterial infections, with patients at risk of sepsis receiving broad-spectrum antibiotics (BSA).

METHODS

The saliva samples were analyzed with shotgun DNA metagenomics and respiratory RNA virome sequencing. Medical records for the period of hospitalization were obtained for all patients. Once hospitalization outcomes were known, patients were classified based on their COVID-19 disease severity and the antibiotics they received.

RESULTS

Our study reveals that BSA regimens differentially impacted the human salivary microbiome and disease progression. 12 patients died and all of them received BSA. Significant associations were found between the composition of the COVID-19 saliva microbiome and BSA use, between SARS-CoV-2 genome coverage and severity of disease. We also found significant associations between the non-bacterial microbiome and severity of disease, with detected most frequently in critical patients. For patients who did not receive BSA before saliva sampling, our study suggests as a potential risk factor for sepsis.

DISCUSSION

Our results indicate that the course of the infection may be explained by both monitoring antibiotic treatment and profiling a patient's salivary microbiome, establishing a compelling link between microbiome and the specific antibiotic type and timing of treatment. This approach can aid with emergency room triage and inpatient management but also requires a better understanding of and access to narrow-spectrum agents that target pathogenic bacteria.

摘要

引言

在新冠病毒德尔塔变异株激增期间,CLAIRE横断面研究对120名住院患者的唾液进行了采样,其中116人的新冠病毒聚合酶链反应(PCR)检测呈阳性。由于可能存在继发性细菌感染,患者入院时接受了抗生素治疗,有败血症风险的患者接受了广谱抗生素(BSA)治疗。

方法

采用鸟枪法DNA宏基因组学和呼吸道RNA病毒组测序对唾液样本进行分析。获取了所有患者的住院期间病历。一旦了解住院结局,就根据患者的新冠病情严重程度和所接受的抗生素对患者进行分类。

结果

我们的研究表明,BSA治疗方案对人类唾液微生物群和疾病进展有不同影响。12名患者死亡,他们均接受了BSA治疗。在新冠唾液微生物群组成与BSA使用之间、严重急性呼吸综合征冠状病毒2(SARS-CoV-2)基因组覆盖率与疾病严重程度之间发现了显著关联。我们还发现非细菌微生物群与疾病严重程度之间存在显著关联,在重症患者中检测到的情况最为频繁。对于在唾液采样前未接受BSA治疗的患者,我们的研究表明 是败血症的一个潜在风险因素。

讨论

我们的结果表明,感染过程可能通过监测抗生素治疗和分析患者的唾液微生物群来解释,从而在微生物群与特定抗生素类型及治疗时机之间建立起令人信服的联系。这种方法有助于急诊室分诊和住院患者管理,但还需要更好地了解和使用针对病原菌的窄谱药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0901/10927822/b16ab99623c2/fmicb-15-1346762-g001.jpg

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