首页> 外文期刊>Heart and Lung: The Journal of Critical Care >Human parainfluenza virus type 3 (HPIV 3) viral community-acquired pneumonia (CAP) mimicking swine influenza (H1N1) during the swine flu pandemic.
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Human parainfluenza virus type 3 (HPIV 3) viral community-acquired pneumonia (CAP) mimicking swine influenza (H1N1) during the swine flu pandemic.

机译:在猪流感大流行期间,人类副流感病毒3型(HPIV 3)模仿了猪流感(H1N1)的社区获得性肺炎(CAP)。

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BACKGROUND: The swine influenza (H1N1) pandemic began in Mexico in 2009 and quickly spread worldwide. During the H1N1 pandemic, many patients were admitted to the Winthrop-University Hospital with influenza-like illnesses (ILIs). Many hospitalized adults had H1N1 pneumonia diagnosed by laboratory or clinical criteria. However, the laboratory diagnosis of H1N1 was problematic. The rapid influenza (QuickVue A/B [Quidel, San Diego, CA]) test frequently showed false-negative results. Reverse transcriptase-polymerase chain reaction (RT-PCR), the definitive test for H1N1, was restricted or unavailable, or results were reported after they were clinically relevant. Because of difficulties making a laboratory diagnosis of H1N1, Winthrop-University Hospital's Infectious Disease Division developed clinical criteria to diagnose H1N1 when rapid influenza diagnostic test (RIDT) results were negative. It also became clear that some patients with negative RIDT and RT-PCR H1N1 clearly had H1N1 pneumonia on a clinical basis. There have been patients who died of H1N1 pneumonia with negative RIDT and RT-PCR H1N1 but had postmortem lung specimens positive for H1N1 by RT-PCR. METHODS: During the flu pandemic, the main diagnostic and infection control problems were to differentiate ILIs from H1N1. Unlike admitted adults hospitalized with ILIs, clinical H1N1 pneumonia patients with negative RIDT results but had dry cough, myalgias, temperatures greater than 102 degrees F, and a negative chest x-ray without focal segmental/lobar infiltrates. With the use of the Winthrop-University Hospital's Infectious Disease Division diagnostic H1N1 triad, patients with H1N1 had the above plus 3 of the following 4 laboratory abnormalities: relative lymphopenia, thrombocytopenia, elevated serum transaminases, or elevated creatine phosphokinase. It was important to rapidly and accurately diagnose H1N1 to place such patients on proper precautions and initiate oseltamivir therapy. RESULTS: As the H1N1 pandemic progressed, it became clear that there were some infectious diseases that mimicked H1N1 pneumonia (eg, Legionnaires' disease). We describe the case of a 61-year-old man who presented with an ILI with dry cough, fever, myalgias, and shortness of breath. His rapid influenza A test result was negative, and specimens for RT-PCR for H1N1 were ordered. On admission, he had relative lymphopenia, thrombocytopenia, and an elevated creatine phosphokinase. His chest x-ray showed no focal segmental or lobar infiltrates. The patient was placed on influenza precautions and administered oseltamivir. During the patient's hospital course, the RT-PCR for H1N1 was reported negative. His respiratory fluorescent antibody viral panel was negative for influenza A, influenza B, metapneumoviruses, respiratory syncytial virus, and adenoviruses but positive for human parainfluenza virus type 3 (HPIV 3). CONCLUSIONS: Clinicians should be aware of other causes of community-acquired pneumonia that may mimic H1N1 pneumonia. In our experience, the most common mimics of H1N1 pneumonia are Legionnaires' disease or HPIV 3 in adults, and metapneumovirus or respiratory syncytial virus in children. In adult patients who present with an ILI and negative RIDT results, we suggest that respiratory secretions specimens be obtained for respiratory fluorescent antibody viral testing pending RT-PCR for H1N1 results. HPIV 3, known to be an important community-acquired pneumonia pathogen in transplant recipients and immunosuppressed patients, is also an important pathogen in immunocompetent adults. In normal adult hosts, the clinical presentation of HPIV 3 pneumonia may clinically closely mimic H1N1 pneumonia.
机译:背景:猪流感(H1N1)大流行于2009年在墨西哥开始,并迅速传播到世界各地。在H1N1大流行期间,许多患者因流感样疾病(ILIs)被送入温思罗普大学医院。根据实验室或临床标准,许多住院的成年人患有H1N1肺炎。但是,H1N1的实验室诊断存在问题。快速流感(QuickVue A / B [Quidel,圣地亚哥,加利福尼亚])测试经常显示假阴性结果。逆转录酶-聚合酶链反应(RT-PCR)(H1N1的权威性检测)受到限制或无法使用,或者在临床上有相关性后才报告结果。由于难以对H1N1进行实验室诊断,温斯罗普大学医院的传染病科制定了快速流感诊断检测(RIDT)结果为阴性时诊断H1N1的临床标准。同样清楚的是,在临床上,一些RIDT和RT-PCR H1N1阴性的患者显然患有H1N1肺炎。有些患者死于H1N1肺炎,其RIDT和RT-PCR H1N1阴性,但死后肺标本经RT-PCR阳性。方法:在流感大流行期间,主要的诊断和感染控制问题是区分ILI和H1N1。与住院接受ILI的成人不同,临床H1N1肺炎患者的RIDT结果为阴性,但有干咳,肌痛,体温高于102华氏度,且胸部X射线检查阴性,无局灶性节段性/大叶浸润。通过使用温斯罗普大学医院传染病科诊断的H1N1三联征,H1N1患者具有以下4种实验室异常中的3种:相对淋巴细胞减少症,血小板减少症,血清转氨酶升高或肌酸磷酸激酶升高。快速准确地诊断H1N1至关重要,以使此类患者采取适当的预防措施并开始使用oseltamivir治疗。结果:随着H1N1大流行的进展,很明显有些传染病模仿了H1N1肺炎(例如退伍军人病)。我们描述了一个患有ILI且干燥咳嗽,发烧,肌痛和呼吸急促的61岁男性的病例。他的快速甲型流感检测结果为阴性,并订购了用于H1N1的RT-PCR标本。入院时,他有相对的淋巴细胞减少症,血小板减少症和肌酸磷酸激酶升高。他的胸部X光片未显示局灶性节段或大叶浸润。患者接受流感预防,并使用奥司他韦。据报道,在患者的住院期间,H1N1的RT-PCR呈阴性。他的呼吸荧光抗体病毒谱对甲型流感,乙型流感,间质肺病毒,呼吸道合胞病毒和腺病毒呈阴性,而对人副流感病毒3型(HPIV 3)呈阳性。结论:临床医生应注意可能是模仿H1N1肺炎的社区获得性肺炎的其他原因。根据我们的经验,H1N1肺炎的最常见模拟物是成年人中的军团病或HPIV 3,儿童中的肺炎病毒或呼吸道合胞病毒。对于表现出ILI和RIDT阴性的成年患者,我们建议获得呼吸道分泌物标本,以进行H1N1结果的RT-PCR呼吸荧光抗体病毒测试。 HPIV 3,众所周知是移植受者和免疫抑制患者中重要的社区获得性肺炎病原体,也是具有免疫能力的成年人中的重要病原体。在正常的成年宿主中,HPIV 3肺炎的临床表现可能在临床上模仿H1N1肺炎。

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