Haemophilus influenzae

流感嗜血杆菌
  • 文章类型: Journal Article
    流感嗜血杆菌血清型a(Hia)最近已成为北美北极和亚北极地区侵袭性疾病的重要原因,主要影响土著儿童。在这项研究中,我们解决了Hia和所有流感嗜血杆菌在鼻咽部的患病率是否在侵袭性Hia疾病发病率高和低的地区的儿科人群之间存在差异的问题.使用分子遗传学方法分析了从急性呼吸道感染(ARTI)儿童中收集的鼻咽标本,以进行呼吸道病毒的常规诊断检测,以鉴定和血清型流感嗜血杆菌。在努纳武特,侵袭性Hia病发病率高的地区,在60.6%和3.0%的儿童鼻咽中发现了所有流感嗜血杆菌,特别是Hia。在安大略省南部(汉密尔顿地区),在Hia侵袭性疾病很少见的地方,所有流感嗜血杆菌和Hia的检测频率分别为38.5%和0.6%,分别。在这两个队列中,不可分型的流感嗜血杆菌流行(57.0%和37.9%,分别)。考虑到Hia是努纳武特地区儿童严重侵袭性疾病的重要原因,ARTI儿童中Hia的3%患病率可以反映出北部社区病原体的持续循环,这可能导致侵袭性疾病的爆发。
    Haemophilus influenzae serotype a (Hia) has recently emerged as an important cause of invasive disease in the North American Arctic and Sub-Arctic regions, mainly affecting young Indigenous children. In this study, we addressed the question of whether the prevalence of Hia and all H. influenzae in the nasopharynx differed between paediatric populations from regions with high versus low incidence of invasive Hia disease. Nasopharyngeal specimens from children with acute respiratory tract infections (ARTI) collected for routine diagnostic detection of respiratory viruses were analysed with molecular-genetic methods to identify and serotype H. influenzae. In Nunavut, a region with a high incidence of invasive Hia disease, all H. influenzae and particularly Hia were found in the nasopharynx of 60.6% and 3.0% children. In Southern Ontario (Hamilton region), where Hia invasive disease is rare, the frequencies of all H. influenzae and Hia detection were 38.5% and 0.6%, respectively. In both cohorts, non-typeable H. influenzae was prevalent (57.0% and 37.9%, respectively). Considering that Hia is an important cause of severe invasive disease in Nunavut children, 3% prevalence of Hia among children with ARTI can reflect continuing circulation of the pathogen in the Northern communities that may result in invasive disease outbreaks.
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  • 文章类型: Journal Article
    胸膜脓胸是小儿肺炎的严重并发症。细菌培养阴性通常会阻碍最佳抗生素治疗。为了提高细菌鉴定,我们开发了一种分子检测方法,并与细菌培养进行了比较。我们的多重定量PCR检测肺炎链球菌,化脓性链球菌,使用细菌基因组DNA和实验室制备的样品(n=267)评估了金黄色葡萄球菌和流感嗜血杆菌。为了评估临床表现,我们进行了胸部脓胸分子评估(MATE)观察性研究,登记患有脓胸住院的儿童。通过细菌培养和多重qPCR检测胸膜液,和使用研究黄金标准确定的性能。我们确定了临床敏感性和时间到生物体的鉴定,以评估多重qPCR减少经验性非靶向抗生素治疗持续时间的潜力。使用加标样品,多重qPCR对所有生物体均表现出213/215(99.1%)的敏感性和52/52(100%)的特异性.在2019年5月至2023年3月期间,有100名儿童参加了MATE研究;平均年龄为3.9岁(IQR2-5.6)。通过多重qPCR在90/100(90%)标本中鉴定出细菌病原体,细菌培养24/100(24%)(P<0.001)。多重qPCR在68/76(90%)培养阴性标本中鉴定出细菌原因。肺炎链球菌是最常见的病原体,在67/100(67%)标本中鉴定。我们估计我们的多重qPCR将减少61%病例中非靶向抗生素治疗的持续时间,中位数为20天(IQR17.5-23,范围1-55)。与培养物相比,多重qPCR显着增加了病原体检测,并且可以减少非靶向抗生素治疗的持续时间。
    Pleural empyema is a serious complication of pneumonia in children. Negative bacterial cultures commonly impede optimal antibiotic therapy. To improve bacterial identification, we developed a molecular assay and evaluated its performance compared with bacterial culture. Our multiplex-quantitative PCR to detect Streptococcus pneumoniae, Streptococcus pyogenes, Staphylococcus aureus and Haemophilus influenzae was assessed using bacterial genomic DNA and laboratory-prepared samples (n = 267). To evaluate clinical performance, we conducted the Molecular Assessment of Thoracic Empyema (MATE) observational study, enrolling children hospitalised with empyema. Pleural fluids were tested by bacterial culture and multiplex-qPCR, and performance determined using a study gold standard. We determined clinical sensitivity and time-to-organism-identification to assess the potential of the multiplex-qPCR to reduce the duration of empiric untargeted antibiotic therapy. Using spiked samples, the multiplex-qPCR demonstrated 213/215 (99.1%) sensitivity and 52/52 (100%) specificity for all organisms. During May 2019-March 2023, 100 children were enrolled in the MATE study; median age was 3.9 years (IQR 2-5.6). A bacterial pathogen was identified in 90/100 (90%) specimens by multiplex-qPCR, and 24/100 (24%) by bacterial culture (P <0.001). Multiplex-qPCR identified a bacterial cause in 68/76 (90%) culture-negative specimens. S. pneumoniae was the most common pathogen, identified in 67/100 (67%) specimens. We estimate our multiplex-qPCR would have reduced the duration of untargeted antibiotic therapy in 61% of cases by a median 20 days (IQR 17.5-23, range 1-55). Multiplex-qPCR significantly increased pathogen detection compared with culture and may allow for reducing the duration of untargeted antibiotic therapy.
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  • 文章类型: Journal Article
    目的:本研究旨在描述三级医院成人社区获得性肺炎(CAP)的微生物病因,并评估综合聚合酶链反应(PCR)对病原体检测的影响。
    方法:在Haukeland大学医院进行,挪威,从2020年9月至2023年4月,这项前瞻性研究纳入了疑似CAP的成年人。我们使用标准护理测试和BIOFIRE®FILMARRAY®肺炎加面板(FAP加)分析了下呼吸道样本。FAPPlus在增强临床相关病原体检测方面的附加价值,除了标准的护理诊断,被评估。
    结果:在筛查的3,238名患者中,640符合纳入标准,384人在出院时确认有CAP。在这些患者中,在312例(81.3%)患者中发现了具有证实或可能的临床意义的病原体.流感嗜血杆菌是最常见的病原体,在118名患者(30.7%)中发现,其次是SARS-CoV-2在74(19.3%),肺炎链球菌64例(16.7%)。在186例(48.4%)患者中检测到呼吸道病毒。FAP的使用将病原体检出率从标准护理方法的62.8%提高到81.3%。
    结论:在81%的CAP患者中发现了病原体,流感嗜血杆菌和呼吸道病毒是最常见的病原体。添加FAPplus面板,与单独的护理诊断标准相比,病原体检出率显着提高。
    OBJECTIVE: This study aimed to describe the microbial aetiology of community-acquired pneumonia (CAP) in adults admitted to a tertiary care hospital and assess the impact of syndromic polymerase chain reaction (PCR) panels on pathogen detection.
    METHODS: Conducted at Haukeland University Hospital, Norway, from September 2020 to April 2023, this prospective study enrolled adults with suspected CAP. We analysed lower respiratory tract samples using both standard-of-care tests and the BIOFIRE® FILMARRAY® Pneumonia Plus Panel (FAP plus). The added value of FAP Plus in enhancing the detection of clinically relevant pathogens, alongside standard-of-care diagnostics, was assessed.
    RESULTS: Of the 3238 patients screened, 640 met the inclusion criteria, with 384 confirmed to have CAP at discharge. In these patients, pathogens with proven or probable clinical significance were identified in 312 (81.3%) patients. Haemophilus influenzae was the most prevalent pathogen, found in 118 patients (30.7%), followed by SARS-CoV-2 in 74 (19.3%), and Streptococcus pneumoniae in 64 (16.7%). Respiratory viruses were detected in 186 (48.4%) patients. The use of FAP plus improved the pathogen detection rate from 62.8% with standard-of-care methods to 81.3%.
    CONCLUSIONS: Pathogens were identified in 81% of CAP patients, with Haemophilus influenzae and respiratory viruses being the most frequently detected pathogens. The addition of the FAP plus panel, markedly improved pathogen detection rates compared to standard-of-care diagnostics alone.
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  • 文章类型: Journal Article
    UNASSIGNED: Haemophilus influenzae serotype a (Hia) has recently emerged as an important cause of invasive disease, mainly affecting young Indigenous children. Carriage of H. influenzae is a pre-requisite for invasive disease and reservoir for transmission. To better understand the epidemiology of invasive Hia disease, we initiated a multicentre study of H. influenzae nasopharyngeal carriage among Canadian children.
    UNASSIGNED: With prior parental consent, we collected nasotracheal tubes used during general anaesthesia in healthy children following routine dental surgery in a regional hospital of northwestern Ontario and a dental clinic in central Saskatchewan. In northwestern Ontario, all children were Indigenous (median age 48.0 months, 45.8% female); in Saskatchewan, children were from various ethnic groups (62% Indigenous, median age 56.3 months, 43.4% female). Detection of H. influenzae and serotyping were performed using molecular-genetic methods.
    UNASSIGNED: A total of 438 nasopharyngeal specimens, 286 in northwestern Ontario and 152 in Saskatchewan were analyzed. Hia was identified in 26 (9.1%) and 8 (5.3%) specimens, respectively. In Saskatchewan, seven out of eight children with Hia carriage were Indigenous.
    UNASSIGNED: The carriage rates of Hia in healthy children in northwestern Ontario and Saskatchewan are comparable to H. influenzae serotype b (Hib) carriage among Alaska Indigenous children in the pre-Hib-vaccine era. To prevent invasive Hia disease, paediatric conjugate Hia vaccines under development have the potential to reduce carriage of Hia, and thus decrease the risk of transmission and disease among susceptible populations. Addressing the social determinants of health may further eliminate conditions favouring Hia transmission in Indigenous communities.
    UNASSIGNED: L’Haemophilus influenzae de sérotype a (Hia) a récemment émergé comme une cause importante de maladie invasive, particulièrement chez les jeunes enfants autochtones. Il faut être porteur de l’H. influenzae pour contracter une maladie invasive et devenir un réservoir de transmission. Pour mieux comprendre l’épidémiologie de l’infection invasive à Hia, les chercheurs ont lancé une étude multicentrique sur le portage nasopharyngé de l’H. influenzae chez les enfants canadiens.
    UNASSIGNED: Après avoir obtenu le consentement des parents, les chercheurs ont recueilli les sondes nasotrachéales utilisées pendant l’anesthésie générale chez des enfants en santé après une chirurgie dentaire courante dans un hôpital régional du nord-ouest de l’Ontario et une clinique dentaire du centre de la Saskatchewan. Dans le nord-ouest de l’Ontario, tous les enfants étaient autochtones (âge médian de 48,0 mois, 45,8 % de filles); en Saskatchewan, les enfants provenaient de divers groupes ethniques (62 % d’Autochtones, âge médian de 56,3 mois, 43,4 % de femmes). La détection de l’H. influenzae et le sérotypage ont été effectués au moyen de méthodes de génétique moléculaire.
    UNASSIGNED: Au total, les chercheurs ont analysé 438 échantillons nasopharyngés, soit 286 du nord-ouest de l’Ontario et 152 de la Saskatchewan. L’Hia a été décelé dans 26 (9,1 %) et huit (5,3 %) échantillons, respectivement. En Saskatchewan, sept des huit enfants porteurs de l’Hia étaient autochtones.
    UNASSIGNED: Le taux de portage de l’Hia chez les enfants en santé du nord-ouest de l’Ontario et de la Saskatchewan était comparable à celui du portage de l’H. influenzae du sérotype b (Hib) chez les enfants autochtones de l’Alaska avant le déploiement des vaccins contre le Hib. Pour éviter l’infection invasive à Hia, les vaccins pédiatriques conjugués contre l’Hia en cours de développement peuvent réduire le portage de l’Hia, et donc le risque de transmission et de maladie dans les populations susceptibles. Le fait d’aborder les déterminants sociaux de la santé pourrait contribuer à éliminer les conditions favorables à la transmission à Hia dans les communautés autochtones.
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  • 文章类型: Journal Article
    背景:细菌定植是支气管扩张的一个重要方面。尽管流感嗜血杆菌在某些地区是一种常见的定植者,其临床影响知之甚少。本研究旨在阐明流感嗜血杆菌定植对支气管扩张患者的影响。
    方法:这项回顾性研究筛选了2003年4月1日至2021年5月16日在韩国三级转诊中心诊断为支气管扩张的成年患者。倾向评分匹配用于匹配有和没有流感嗜血杆菌定植的患者。我们根据支气管扩张严重程度指数评估支气管扩张的严重程度,恶化的发生率,肺功能的差异,和全因死亡率。
    结果:在4,453例支气管扩张患者中,79例(1.8%)被流感嗜血杆菌定植。1:2倾向得分匹配后,从流感嗜血杆菌定植者和非定植者组中选择78和154例患者,分别。尽管两组之间在基线人口统计方面没有显着差异,流感嗜血杆菌定植的患者的支气管扩张严重程度指数较高(中位数6[四分位距4-8]与4[2-7],p=0.002),与广泛的影像学检查相关(52.2%vs.37.2%,p=0.045)和未住院的轻度加重(调整后的发生率比0.15;95%置信区间0.12-0.24)。肺功能和死亡率没有显着差异,不管流感嗜血杆菌定植。
    结论:H.支气管扩张的流感定植与更严重的疾病和更高的轻度恶化发生率相关。但不是肺功能和死亡率。支气管扩张伴流感嗜血杆菌定植的患者应注意。
    BACKGROUND: Bacterial colonization is an essential aspect of bronchiectasis. Although Haemophilus influenzae is a frequent colonizer in some regions, its clinical impacts are poorly understood. This study aimed to elucidate the impact of H. influenzae colonization in patients with bronchiectasis.
    METHODS: This retrospective study screened adult patients diagnosed with bronchiectasis at a tertiary referral center between April 1, 2003, and May 16, 2021, in South Korea. Propensity score matching was used to match patients with and without H. influenzae colonization. We assessed the severity of bronchiectasis as per the bronchiectasis severity index, the incidence of exacerbation, differences in lung function, and all-cause mortality.
    RESULTS: Out of the 4,453 patients with bronchiectasis, 79 (1.8%) were colonized by H. influenzae. After 1:2 propensity score matching, 78 and 154 patients were selected from the H. influenzae colonizer and non-colonizer groups, respectively. Although there were no significant differences between the groups regarding baseline demographics, patients colonized with H. influenzae had a higher bronchiectasis severity index (median 6 [interquartile range 4-8] vs. 4 [2-7], p = 0.002), associated with extensive radiographic involvement (52.2% vs. 37.2%, p = 0.045) and mild exacerbation without hospitalization (adjusted incidence rate ratio 0.15; 95% confidence interval 0.12-0.24). Lung function and mortality rates did not reveal significant differences, regardless of H. influenzae colonization.
    CONCLUSIONS: H. influenzae colonization in bronchiectasis was associated with more severe disease and greater incidence of mild exacerbation, but not lung function and mortality. Attention should be paid to patients with bronchiectasis with H. influenzae colonization.
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  • 文章类型: Observational Study
    背景:在COVID-19大流行期间部署非药物干预措施,如面部掩蔽和身体远离,可能改变了呼吸道生物的传播动力学和携带。我们评估了在COVID-19大流行之前和期间肺炎链球菌和其他上呼吸道细菌定植者的定植。
    方法:我们在索韦托进行了两次横断面调查,南非2018年7月3日至12月13日(COVID-19前)和2021年8月4日至2022年3月31日(COVID-19期间)健康儿童(年龄≤60个月)在招募前21天未接受抗生素治疗。在入学时,我们收集了儿童参与者的鼻咽拭子样本.核酸提取后,使用纳米流体定量PCR筛选所有样品中的92种肺炎链球菌血清型和14种其他细菌。主要目的是比较肺炎球菌鼻咽部定植的患病率和密度。按13价肺炎球菌结合疫苗(PCV13)血清型和非疫苗血清型进行总体和分层。次要研究目标包括血清型特异性肺炎球菌定植和密度的比较,以及与COVID-19前期相比,其他14种细菌在COVID-19中的定殖。我们使用调整后的多元逻辑和线性回归模型来比较研究期间的定植患病率和密度。
    结果:我们分析了1107名儿童的鼻咽拭子(COVID-19前期的n=571;COVID-19期的n=536)。我们观察到各期之间的总体肺炎球菌定植没有变化(COVID-19期536例中的274[51%]与COVID-19期前571例中的282[49%];调整后比值比[aOR]1·03[95%CI0·95-1·12])。COVID-19中PCV13血清型的患病率低于COVID-19前期(72[13%]对106[19%];0·87[0·78-0·97]),而不可分型肺炎链球菌的患病率较高(34[6%]vs63[12%];1·30[1·12-1·50])。COVID-19期肺炎球菌总体定植的平均log10密度低于COVID-19前期(3·96[95%CI3·85-4·07]vs4·72[4·63-4·80]log10基因组当量/mL;p<0·0001)。非疫苗血清型的密度较低(3·63[3·51-3·74]vs4·08[3·95-4·22]log10基因组当量/mL;p<0·0001)和不可分型的肺炎链球菌(3·11[2·94-3·29]vs4·41[4·06-4·75]log10基因组当量/mL;在CO00V19中也观察到p<0·这两个时期之间的PCV13血清型密度没有差异。不可分型流感嗜血杆菌在COVID-19期间的定植率低于COVID-19之前(280[49%]对165[31%];aOR0·77[95%CI0·71-0·84]),卡他莫拉菌(328[57%]对242[45%];0·85[0·79-0·92]),和内酰菌(51[9%]对13[2%];0·64[0·52-0·78]),但较高的鲍曼不动杆菌(34[6%]对102[19%];1·55[1·35-1·77])和金黄色葡萄球菌(29[5%]对52[10%];1·28[1·10-1·50])。
    结论:与COVID-19前期相比,COVID-19期间对细菌的定植患病率和密度有不同的影响。PCV13血清型的较低患病率以及其他呼吸道生物,包括不可分型的流感嗜血杆菌和粘膜炎菌,可能在一定程度上导致了在COVID-19大流行初期在南非观察到的全因下呼吸道感染的减少。鲍曼不动杆菌和金黄色葡萄球菌定植增加的病理生理机制值得进一步研究。这些发现的临床相关性也是如此。
    背景:比尔和梅琳达·盖茨基金会。
    Deployment of non-pharmaceutical interventions such as face masking and physical distancing during the COVID-19 pandemic could have altered the transmission dynamics and carriage of respiratory organisms. We evaluated colonisation with Streptococcus pneumoniae and other upper respiratory tract bacterial colonisers before and during the COVID-19 pandemic.
    We did two cross-sectional surveys in Soweto, South Africa from July 3 to Dec 13, 2018 (pre-COVID-19 period) and from Aug 4, 2021, to March 31, 2022 (COVID-19 period) in healthy children (aged ≤60 months) who had recorded HIV status and had not received antibiotics in the 21 days before enrolment. At enrolment, we collected nasopharyngeal swab samples from child participants. Following nucleic acid extraction, nanofluidic quantitative PCR was used to screen all samples for 92 S pneumoniae serotypes and 14 other bacteria. The primary objective was to compare the prevalence and density of pneumococcal nasopharyngeal colonisation, overall and stratified by 13-valent pneumococcal conjugate vaccine (PCV13) serotypes and non-vaccine serotypes. Secondary study objectives included a comparison of serotype-specific pneumococcal colonisation and density, as well as colonisation by the 14 other bacteria in the COVID-19 versus pre-COVID-19 period. We used an adjusted multiple logistic and linear regression model to compare the colonisation prevalence and density between study periods.
    We analysed nasopharyngeal swabs from 1107 children (n=571 in the pre-COVID-19 period; n=536 in the COVID-19 period). We observed no change in overall pneumococcal colonisation between periods (274 [51%] of 536 in the COVID-19 period vs 282 [49%] of 571 in the pre-COVID-19 period; adjusted odds ratio [aOR] 1·03 [95% CI 0·95-1·12]). The prevalence of PCV13 serotypes was lower in the COVID-19 than in the pre-COVID-19 period (72 [13%] vs 106 [19%]; 0·87 [0·78-0·97]), whereas the prevalence of non-typeable S pneumoniae was higher (34 [6%] vs 63 [12%]; 1·30 [1·12-1·50]). The mean log10 density for overall pneumococcal colonisation was lower in the COVID-19 period than in the pre-COVID-19 period (3·96 [95% CI 3·85-4·07] vs 4·72 [4·63-4·80] log10 genome equivalents per mL; p<0·0001). A lower density of non-vaccine serotypes (3·63 [3·51-3·74] vs 4·08 [3·95-4·22] log10 genome equivalents per mL; p<0·0001) and non-typeable S pneumoniae (3·11 [2·94-3·29] vs 4·41 [4·06-4·75] log10 genome equivalents per mL; p<0·00001) was also observed in the COVID-19 period. There was no difference in the density of PCV13 serotypes between the periods. The prevalence of colonisation during the COVID-19 versus pre-COVID-19 period was lower for non-typeable Haemophilus influenzae (280 [49%] vs 165 [31%]; aOR 0·77 [95% CI 0·71-0·84]), Moraxella catarrhalis (328 [57%] vs 242 [45%]; 0·85 [0·79-0·92]), and Neisseria lactamica (51 [9%] vs 13 [2%]; 0·64 [0·52-0·78]), but higher for Acinetobacter baumannii (34 [6%] vs 102 [19%]; 1·55 [1·35-1·77]) and Staphylococcus aureus (29 [5%] vs 52 [10%]; 1·28 [1·10-1·50]).
    There were variable effects on the colonisation prevalence and density of bacterial organisms during the COVID-19 compared with the pre-COVID-19 period. The lower prevalence of PCV13 serotype together with other respiratory organisms including non-typeable H influenzae and M catarrhalis could have in part contributed to a decrease in all-cause lower respiratory tract infections observed in South Africa during the initial stage of the COVID-19 pandemic. The pathophysiological mechanism for the increase in A baumannii and S aureus colonisation warrants further investigation, as does the clinical relevance of these findings.
    The Bill & Melinda Gates Foundation.
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  • 文章类型: Case Reports
    在这个比较案例研究中,我们讨论了头孢曲松抗菌药敏试验(AST)解释的临床相关差异,β-内酰胺酶阴性,从血液培养物中分离的氨苄西林抗性(BLNAR)流感嗜血杆菌。
    一名74岁的男子患有3天的疾病,其特征是呼吸急促和干咳,入院时发热和缺氧。血培养瓶标记为革兰氏阴性球杆菌阳性,后来被确定为流感嗜血杆菌的患者开始使用头孢曲松。分离株为β-内酰胺酶阴性,使用圆盘扩散进行的抗生素敏感性测试(AST)显示,通过EUCAST方法,分离株对头孢曲松和氨苄西林具有抗性。患者随后改为阿莫西林/克拉维酸。并行使用CLSI方法的进一步AST证明了两种敏感性方法之间的差异结果。患者康复,无并发症。
    这种差异可能导致实验室之间的敏感性报告不一致,因此抗生素处方,特别是对于侵入性分离物。随着越来越多的实验室在澳大利亚和全球采用EUCAST方法进行AST解释,临床医生必须考虑这些方法学差异的临床意义.
    UNASSIGNED: In this comparative case study, we discuss clinically relevant discrepancies of antimicrobial susceptibility testing (AST) interpretation for ceftriaxone against a non-typable, beta-lactamase negative, ampicillin-resistant (BLNAR) Haemophilus influenzae isolated from a blood culture.
    UNASSIGNED: A 74-year-old man presented with a 3 day illness characterized by shortness of breath and dry cough, and was noted to be febrile and hypoxic on admission. A blood culture bottle flagged positive with Gram-negative coccobacilli, later identified as Haemophilus influenzae with the patient commenced on ceftriaxone. The isolate was beta-lactamase negative and antibiotic susceptibility testing (AST) using disc diffusion revealed the isolate resistant to ceftriaxone and ampicillin by EUCAST methodology, with the patient subsequently changed to amoxicillin/clavulanate. Further AST using the CLSI methodology in parallel demonstrated discrepant results between the two susceptibility methods. The patient recovered without complications.
    UNASSIGNED: This discrepancy could lead to inconsistent reporting of susceptibilities between laboratories, and consequently antibiotic prescribing, especially for invasive isolates. As more laboratories adopt EUCAST methodologies for AST interpretation in Australia and globally, it is important for clinicians to consider the clinical implications of these methodological discrepancies.
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  • 文章类型: Journal Article
    急性鼻窦炎和病毒性上呼吸道感染症状之间的大量重叠表明某些亚组儿童被诊断为急性鼻窦炎,随后用抗生素治疗,从抗生素使用中获益甚微。
    评估在预先指定的亚组中是否可以适当地停止抗生素治疗。
    随机临床试验,包括515名根据临床标准诊断为急性鼻窦炎的2至11岁儿童。该试验于2016年2月至2022年4月在美国6家机构的初级保健办公室进行,旨在评估由鼻咽肺炎链球菌定义的亚组的症状负担是否不同。流感嗜血杆菌,或卡他莫拉氏菌在细菌培养和彩色鼻腔分泌物的存在。
    口服阿莫西林(90mg/kg/d)和克拉维酸(6.4mg/kg/d)(n=254)或安慰剂(n=256)10天。
    主要结局是基于经过验证的量表上的每日症状评分的症状负担(范围,0-40)在诊断后的10天内。次要结果包括治疗失败,不良事件包括临床上显著的腹泻,和家庭使用资源。
    510名儿童中的大多数年龄在2至5岁之间(64%),男性(54%)白色(52%),而不是西班牙裔(89%)。与安慰剂组(10.60[95%CI,10.27至10.93])相比,阿莫西林和克拉维酸组儿童的平均症状评分显著降低(9.04[95%CI,8.71至9.37])(组间差异,-1.69[95%CI,-2.07至-1.31])。抗生素组(7.0天)的儿童症状缓解时间明显低于安慰剂组(9.0天)(P=.003)。没有检测到鼻咽病原体的儿童从抗生素治疗中获益不如有检测到病原体的儿童;没有检测到病原体的患者的平均症状评分的组间差异为-0.88(95%CI,-1.63至-0.12),而有检测到病原体的患者为-1.95(95%CI,-2.40至-1.51)。根据是否存在有色鼻分泌物,疗效没有显着差异(有色鼻分泌物的组间差异为-1.62[95%CI,-2.09至-1.16],而透明鼻分泌物的组间差异为-1.70[95%CI,-2.38至-1.03];治疗组与有色鼻分泌物的存在之间的相互作用P=.52)。
    在患有急性鼻窦炎的儿童中,抗生素治疗对那些没有鼻咽细菌病原体的患者的益处微乎其微,其效果并不取决于鼻腔分泌物的颜色。测试特定的细菌可能代表了在这种情况下减少抗生素使用的策略。
    ClinicalTrials.gov标识符:NCT02554383。
    The large overlap between symptoms of acute sinusitis and viral upper respiratory tract infection suggests that certain subgroups of children being diagnosed with acute sinusitis, and subsequently treated with antibiotics, derive little benefit from antibiotic use.
    To assess if antibiotic therapy could be appropriately withheld in prespecified subgroups.
    Randomized clinical trial including 515 children aged 2 to 11 years diagnosed with acute sinusitis based on clinical criteria. The trial was conducted between February 2016 and April 2022 at primary care offices affiliated with 6 US institutions and was designed to evaluate whether symptom burden differed in subgroups defined by nasopharyngeal Streptococcus pneumoniae, Haemophilus influenzae, or Moraxella catarrhalis on bacterial culture and by the presence of colored nasal discharge.
    Oral amoxicillin (90 mg/kg/d) and clavulanate (6.4 mg/kg/d) (n = 254) or placebo (n = 256) for 10 days.
    The primary outcome was symptom burden based on daily symptom scores on a validated scale (range, 0-40) during the 10 days after diagnosis. Secondary outcomes included treatment failure, adverse events including clinically significant diarrhea, and resource use by families.
    Most of the 510 included children were aged 2 to 5 years (64%), male (54%), White (52%), and not Hispanic (89%). The mean symptom scores were significantly lower in children in the amoxicillin and clavulanate group (9.04 [95% CI, 8.71 to 9.37]) compared with those in the placebo group (10.60 [95% CI, 10.27 to 10.93]) (between-group difference, -1.69 [95% CI, -2.07 to -1.31]). The length of time to symptom resolution was significantly lower for children in the antibiotic group (7.0 days) than in the placebo group (9.0 days) (P = .003). Children without nasopharyngeal pathogens detected did not benefit from antibiotic treatment as much as those with pathogens detected; the between-group difference in mean symptom scores was -0.88 (95% CI, -1.63 to -0.12) in those without pathogens detected compared with -1.95 (95% CI, -2.40 to -1.51) in those with pathogens detected. Efficacy did not differ significantly according to whether colored nasal discharge was present (the between-group difference was -1.62 [95% CI, -2.09 to -1.16] for colored nasal discharge vs -1.70 [95% CI, -2.38 to -1.03] for clear nasal discharge; P = .52 for the interaction between treatment group and the presence of colored nasal discharge).
    In children with acute sinusitis, antibiotic treatment had minimal benefit for those without nasopharyngeal bacterial pathogens on presentation, and its effects did not depend on the color of nasal discharge. Testing for specific bacteria on presentation may represent a strategy to reduce antibiotic use in this condition.
    ClinicalTrials.gov Identifier: NCT02554383.
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  • 文章类型: Journal Article
    背景:侵袭性流感嗜血杆菌血清型(Hia)疾病很少见,报告的大多数病例来自北美的土著居民。在英国,自2016-17流行病学年以来,实验室确诊的侵袭性Hia病增加,国家监测得到加强.这项研究旨在描述流行病学趋势,病例的临床特征,并评估潜在的基因组驱动因素。
    方法:英格兰的医院实验室常规向英国卫生安全局提交侵袭性流感嗜血杆菌分离株进行确认和血清分型。在这项前瞻性国家监测研究中,我们联系了2008-09年至2021-22年流行病学年度所有实验室确诊的侵袭性Hia患者的全科医生和临床医生,以完成关于人口统计学的临床问卷。潜在条件,临床表现,并发症,结果,以及患者的旅行史。来自英格兰居民的所有Hia侵入性分离株都包括在研究中;非侵入性分离株被排除。多位点序列分型(MLST),全基因组单核苷酸多态性,在Illumina全基因组测序(WGS)之后进行细菌分离物的基于k聚体的分析。结果包括流行病学趋势,确诊Hia病例的临床特征,和基因组分析。
    结果:从2008-09到2021-22流行病学年,英国有52例流感嗜血杆菌血清型a的侵袭性感染(女性患者25例[48%],男性患者27例[52%]).在2015-16年之前,每年有零至两例Hia病例(占血清型流感嗜血杆菌分离株的<0·5%),此后,英格兰的病例在2021-22年增加到19例(每100000例发病率为0·03例),当Hia占484株血清分型的流感嗜血杆菌中的19株(4%)时,100例包囊病例中有19例(19%),在2008-09年至2021-22年期间,所有流感嗜血杆菌病例中有37%(52例中的19例)。最近病例增加的大部分发生在65岁及以上的个人(52人中有17人[33%]),通常出现细菌性肺炎(17人中有13人[76%]),1岁以下的婴儿,发病率最高,更有可能出现脑膜炎(十分之五[50%])。总病死率为7·7%(95%CI2·1-19·7;52例患者中有4例)。WGS发现密切相关的MLST序列类型ST1511(51个中的20[39%]),ST23(51个中的13个[25%]),ST56(51个中的7个[14%])占大多数病例,没有血清型b菌株将胶囊转换为Hia的证据。重复的胶囊操纵子,与更严重的疾病相关,存在于40种这些序列类型中的32种(80%)中。对核心和辅助基因组含量的分析将大多数分离株分为单个菌株。
    结论:英格兰和所有年龄段的侵袭性Hia病例持续增加表明传播广泛,与其他欧洲国家的报道一致,需要密切监测.
    背景:英国卫生安全局。
    Invasive Haemophilus influenzae serotype a (Hia) disease is rare, with most cases reported among Indigenous populations in North America. In England, national surveillance was enhanced following an increase in laboratory-confirmed invasive Hia disease since the 2016-17 epidemiological year. This study aimed to describe the epidemiological trends, clinical characteristics of cases, and assess potential genomic drivers.
    Hospital laboratories in England routinely submit invasive H influenzae isolates to the UK Health Security Agency for confirmation and serotyping. In this prospective national surveillance study we contacted the general practitioners and clinicians of all patients with laboratory-confirmed invasive Hia from the 2008-09 to the 2021-22 epidemiological year to complete a clinical questionnaire on demographics, underlying conditions, clinical presentation, complications, outcomes, and travel history of the patient. All Hia invasive isolates from residents in England were included in the study; non-invasive isolates were excluded. Multilocus sequence typing (MLST), whole genome single-nucleotide polymorphism, and k-mer-based analysis of bacterial isolates were performed following Illumina whole-genome sequencing (WGS). Outcomes included epidemiological trends, clinical characteristics of confirmed Hia cases, and genomic analyses.
    From the 2008-09 to the 2021-22 epidemiological years, there were 52 cases of invasive infection with H influenzae serotype a in England (25 [48%] in female patients and 27 [52%] in male patients). There were zero to two annual Hia cases (accounting for <0·5% of serotyped H influenzae isolates) until 2015-16, after which cases increased across England to 19 cases in 2021-22 (incidence 0·03 cases per 100 000), when Hia accounted for 19 (4%) of 484 serotyped H influenzae isolates, 19 (19%) of 100 capsulated cases, and 37% (19 of 52) of all H influenzae cases between 2008-09 and 2021-22. Most of the recent increase in cases occurred among individuals aged 65 years and older (17 [33%] of 52), who typically presented with bacteraemic pneumonia (13 [76%] of 17), and infants younger than 1 year, who had the highest incidence and were more likely to present with meningitis (five [50%] of ten). Overall case fatality rate was 7·7% (95% CI 2·1-19·7; four of 52 patients). WGS found that closely related MLST sequence types ST1511 (20 [39%] of 51), ST23 (13 [25%] of 51), and ST56 (seven [14%] of 51) accounted for most cases, with no evidence of serotype b strains switching capsule to Hia. Duplication of the capsule operon, associated with more severe disease, was present in 32 (80%) of 40 of these sequence types. Analysis of the core and accessory genome content grouped most isolates into a single strain.
    The persistent increase in invasive Hia cases across England and across all age groups suggests widespread transmission, consistent with reports from other European countries, and will require close monitoring.
    UK Health Security Agency.
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  • 文章类型: Journal Article
    背景:缺乏急性鼻-鼻窦炎并发症的前瞻性研究,细菌培养很难获得,空气中的过敏作用,病毒和免疫球蛋白水平尚不清楚。目的是研究细菌的作用,病毒,因鼻窦炎住院的儿童过敏和免疫球蛋白。
    方法:斯德哥尔摩的一项前瞻性队列研究,瑞典,18岁以下的儿童,因急性细菌性鼻窦炎住院,从4月1日起,2017年4月1日,2020年。
    结果:包括55名儿童,51%的病毒鼻咽PCR阳性,29%的变态反应致敏试验阳性。与鼻咽相比,中鼻道培养物中细菌生长呈阳性的百分比更高,并且显示出更广泛的细菌。手术中主要细菌为米勒氏链球菌(7/12例),中鼻道化脓性美国(13/52例),鼻咽培养物中的化脓性链球菌和H.流感(分别为8/50例)。在50%的手术病例中,鼻培养为阴性。发现化脓性链球菌与CRP峰值之间存在关联;流感嗜血杆菌与CRP峰值之间存在关联;肺炎链球菌与CRP峰值之间存在关联;并且可能在粘膜炎莫拉菌与IV抗生素使用天数之间存在关联。Further,甲型/乙型流感和化脓性链球菌之间的关联;病毒PCR阳性和较低级别的并发症和峰值CRP;以及流感病毒和较低级别的并发症之间的可能关联。过敏致敏可能与使用IV抗生素的天数增加有关。未发现免疫球蛋白缺乏。
    结论:鼻咽部细菌生长模式似乎存在差异,急性细菌性鼻-鼻窦炎并发症患儿的中鼻道和手术培养。某些病毒的存在和对空气过敏的敏感性似乎在儿童急性细菌性鼻窦炎的并发症中起作用。
    BACKGROUND: Prospective studies of complications due to acute rhinosinusitis are lacking, bacterial cultures are hard to obtain and the role of airborne allergies, viruses and immunoglobulin levels are unclear. The aim was to investigate the role of bacteria, viruses, allergy and immunoglobulins in children hospitalized due to rhinosinusitis.
    METHODS: A prospective cohort study in Stockholm, Sweden, of children up to 18 years of age, hospitalized due to acute bacterial rhinosinusitis, from April 1st, 2017 to April 1st, 2020.
    RESULTS: Of 55 children included, 51% had a positive viral nasopharyngeal PCR and 29% had a positive allergy sensitization test. A higher percentage of middle meatus cultures were positive for bacterial growth compared to nasopharyngeal and displayed a wider array of bacteria. Dominating bacteria were S. milleri in surgical (7/12 cases), S. pyogenes in middle meatus (13/52 cases), and S. pyogenes and H. influenza in nasopharyngeal cultures (8/50 cases respectively). Nasal cultures were negative in 50% of surgical cases. An association was found between S. pyogenes and peak CRP; H. influenzae and peak CRP; S. pneumoniae and peak CRP; and possibly between M. catarrhalis and days of IV antibiotics. Further, an association between influenza A/B and S. pyogenes; a positive viral PCR and lower grade of complication and peak CRP; and a possible association between influenza virus and lower grade of complication. Allergy sensitization was possibly associated with a higher number of days with IV antibiotics. No immunoglobulin deficiencies were found.
    CONCLUSIONS: There seem to be differences in the patterns of bacterial growth in nasopharyngeal, middle meatus and surgical cultures in children with complications to acute bacterial rhinosinusitis. Presence of certain viruses and sensitization to airborne allergies seem to play a role in complications to acute bacterial rhinosinusitis in children.
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