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Impact of antibacterials on subsequent resistance and clinical outcomes in adult patients with viral pneumonia: an opportunity for stewardship

机译:抗菌对病毒性肺炎患者随后抗性和临床结果的影响:管理机会

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IntroductionRespiratory viruses are increasingly recognized as significant etiologies of pneumonia among hospitalized patients. Advanced technologies using multiplex molecular assays and polymerase-chain reaction increase the ability to identify viral pathogens and may ultimately impact antibacterial use.MethodThis was a single-center retrospective cohort study to evaluate the impact of antibacterials in viral pneumonia on clinical outcomes and subsequent multidrug-resistant organism (MDRO) infections/colonization. Patients admitted from March 2013 to November 2014 with positive respiratory viral panels (RVP) and radiographic findings of pneumonia were included. Patients transferred from an outside hospital or not still hospitalized 72 hours after the RVP report date were excluded. Patients were categorized based on exposure to systemic antibacterials: less than 3 days representing short-course therapy and 3 to 10 days being long-course therapy.ResultsA total of 174 patients (long-course, n?=?67; short-course, n?=?28; mixed bacterial-viral infection, n?=?79) were included with most being immunocompromised (56.3 %) with active malignancy the primary etiology (69.4 %). Rhinovirus/Enterovirus (23 %), Influenza (19 %), and Parainfluenza (15.5 %) were the viruses most commonly identified. A total of 13 different systemic antibacterials were used as empiric therapy in the 95 patients with pure viral infection for a total of 466 days-of-therapy. Vancomycin (50.7 %), cefepime (40.3 %), azithromycin (40.3 %), meropenem (23.9 %), and linezolid (20.9 %) were most frequently used. In-hospital mortality did not differ between patients with viral pneumonia in the short-course and long-course groups. Subsequent infection/colonization with a MDRO was more frequent in the long-course group compared to the short-course group (53.2 vs 21.1 %; P?=?0.027).ConclusionThis study found that long-course antibacterial use in the setting of viral pneumonia had no impact on clinical outcomes but increased the incidence of subsequent MDRO infection/colonization.
机译:引入促进病毒越来越被认为是住院患者中肺炎的重要病因。使用多重分子测定和聚合酶链反应的先进技术增加了鉴定病毒病原体的能力,最终可能会影响抗菌剂。方法是单中心回顾性队列研究,以评估临床结果对病毒性肺炎的抗菌剂的影响和随后的多药物的影响。抗性生物(MDRO)感染/殖民化。包括从2013年3月到2014年11月录取的患者,患有阳性呼吸道病毒板(RVP)和肺炎的放射线摄影结果。在RVP报告日期之后,从外部医院转移到外科医院或不住院的患者。患者根据暴露于全身抗菌剂进行分类:少于3天,代表短期治疗,长期治疗3至10天。患者共有174名患者(长期,N?= 67;短期, n?=?28;混合细菌病毒感染,n?=β79)被含有免疫脯(56.3%),活性恶性肿瘤主要病因(69.4%)。鼻病毒/肠病毒(23%),流感(19%)和Parainfluenza(15.5%)是最常见的病毒。总共13种不同的全身抗菌剂被用作95例纯病毒感染患者的经验疗法,共计466天治疗。万古霉素(50.7%),头孢酮(40.3%),二十霉素(40.3%),梅洛涅姆(23.9%),最常使用氟氯吡啶(23.9%)和线唑(20.9%)。在短期过程和长期课程中,病毒性肺炎患者之间的住院死亡率没有差异。与短路过程中的长期组(53.2 vs21.1%; p?= 0.027)。结论,在长期组合中,在长期组合中更频繁地在长期组中频繁频繁(53.2 vs 21.1%)。结论该研究发现,在病毒的环境中使用长期抗菌用途肺炎对临床结果没有影响,但增加了随后的MDRO感染/定植的发病率。

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