Metagenomic next-generation sequencing

宏基因组下一代测序
  • 文章类型: Journal Article
    目的:本研究旨在评估圆锥角膜患者角膜上皮层中病原微生物的存在。方法:从十只圆锥角膜和三个健康对照的角膜上皮样品中提取DNA。使用不可知方法进行宏基因组下一代测序(mNGS)以检测眼部微生物群。结果:宏基因组测序显示,在来自圆锥角膜眼(平均:530)和对照(平均:622)的角膜上皮样品中,微生物读数计数较低,没有统计学显著差异(p=0.29)。变形菌是圆锥角膜和对照样品中的主要门(相对丰度:72%对79%,分别)。结论:圆锥角膜和对照样品之间的总体低微生物读数计数和不同微生物种类的相对丰度的差异不支持慢性角膜感染与圆锥角膜的发病机理有关的假设。这些发现并不排除急性感染可能作为起始事件参与疾病过程的可能性。
    Objectives: This study aims to assess the presence of pathogenic microorganisms in the corneal epithelial layer of keratoconus patients. Methods: DNA was extracted from corneal epithelial samples procured from ten individual keratoconus eyes and three healthy controls. Metagenomic next-generation sequencing (mNGS) was performed to detect ocular microbiota using an agnostic approach. Results: Metagenomic sequencing revealed a low microbial read count in corneal epithelial samples derived from both keratoconus eyes (average: 530) and controls (average: 622) without a statistically significant difference (p = 0.29). Proteobacteria were the predominant phylum in both keratoconus and control samples (relative abundance: 72% versus 79%, respectively). Conclusions: The overall low microbial read count and the lack of difference in the relative abundance of different microbial species between keratoconus and control samples do not support the hypothesis that a chronic corneal infection is implicated in the pathogenesis of keratoconus. These findings do not rule out the possibility that an acute infection may be involved in the disease process as an initiating event.
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  • 文章类型: Journal Article
    背景:与没有COPD的患者相比,患有慢性阻塞性肺疾病(COPD)的社区获得性肺炎(CAP)患者的疾病严重程度和死亡率更高。然而,对有或无COPD的CAP患者下呼吸道微生物组分布的深入研究尚不清楚.
    方法:因此,我们使用宏基因组下一代测序(mNGS)来探索两组之间的微生物组差异。
    结果:共检索到36例无COPDCAP和11例COPDCAP病例。收集支气管肺泡灌洗液(BALF)并使用非靶向mNGS和生物信息学分析进行分析。mNGS显示CAP合并COPD组富含链球菌,普雷沃氏菌,属水平的博德特氏菌和痤疮杆菌,粘胶红花,基因博德特氏菌。6在物种水平。虽然无COPD的CAP组有丰富的Ralstonia,普雷沃氏菌,属水平的链球菌和皮克蒂拉尔斯托,粘胶红花,物种水平的黑色素prevotella。同时,两组之间的α和β微生物组多样性相似.线性判别分析发现,pa-raburkholderia,在无COPD的CAP组中,结核杆菌和人葡萄球菌的含量更高,而中间链球菌的含量更高,星座链球菌,milleri链球菌,CAP合并COPD组镰刀菌较高。
    结论:这些研究结果表明,合并COPD对CAP患者的下气道微生物组有轻微影响。
    BACKGROUND: Community-acquired pneumonia (CAP) patients with chronic obstructive pulmonary disease (COPD) have higher disease severity and mortality compared to those without COPD. However, deep investigation into microbiome distribution of lower respiratory tract of CAP with or without COPD was unknown.
    METHODS: So we used metagenomic next generation sequencing (mNGS) to explore the microbiome differences between the two groups.
    RESULTS: Thirty-six CAP without COPD and 11 CAP with COPD cases were retrieved. Bronchoalveolar lavage fluid (BALF) was collected and analyzed using untargeted mNGS and bioinformatic analysis. mNGS revealed that CAP with COPD group was abundant with Streptococcus, Prevotella, Bordetella at genus level and Cutibacterium acnes, Rothia mucilaginosa, Bordetella genomosp. 6 at species level. While CAP without COPD group was abundant with Ralstonia, Prevotella, Streptococcus at genus level and Ralstonia pickettii, Rothia mucilaginosa, Prevotella melaninogenica at species level. Meanwhile, both alpha and beta microbiome diversity was similar between groups. Linear discriminant analysis found that pa-raburkholderia, corynebacterium tuberculostearicum and staphylococcus hominis were more enriched in CAP without COPD group while the abundance of streptococcus intermedius, streptococcus constellatus, streptococcus milleri, fusarium was higher in CAP with COPD group.
    CONCLUSIONS: These findings revealed that concomitant COPD have an mild impact on lower airway microbiome of CAP patients.
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  • 文章类型: Journal Article
    目的:宏基因组下一代测序(mNGS)已广泛应用于感染性疾病的诊断。然而,使用mNGS检测马尔尼菲塔拉酵母的研究仍然很少。因此,本研究旨在探讨mNGS在马尔尼菲氏杆菌中的诊断性能。
    方法:在2021年3月至2023年6月之间,最终诊断为塔拉真菌病的出院患者,或者被mNGS证实了马尔尼菲T.本研究包括培养或病理检查.对所有患者同时进行培养和mNGS。检索临床数据用于分析。
    结果:共纳入78例患者,塔拉真菌病组40例,疑似塔拉真菌病组38例。在塔拉真菌病组中,mNGS的阳性率(40/40,100.0%)高于培养(34/40,85.0%)(P=0.111)。所有的患者在可疑的距骨真菌病组通过培养检测阴性,而mNGS产生了积极的结果。距骨真菌病组的马内菲菌读数显着高于可疑的距骨真菌病组(4399vs.28,P<0.001)。在疑似塔拉真菌病组中,在四名没有接受抗真菌治疗的低读数患者中,1例死亡,1例肺部病变进展;大多数患者(31/34,91.2%)在接受适当的抗真菌治疗后康复.
    结论:mNGS被证明是一种快速和高度灵敏的检测马尔尼菲的方法。较高的马内菲木霉读段对应于较高的感染可能性。然而,低读数的情况需要一个全面的方法,整合临床表现,实验室测试,和影像学检查以确认马尔尼菲氏杆菌感染。
    OBJECTIVE: Metagenomic next-generation sequencing (mNGS) has been widely used in the diagnosis of infectious diseases. However, studies on Talaromyces marneffei detection using mNGS remain scarce. Therefore, this study aimed to explore the diagnostic performance of mNGS in T. marneffei.
    METHODS: Between March 2021 and June 2023, patients who were discharged with a final diagnosis of talaromycosis, or confirmed T. marneffei infection by mNGS, culture or pathological examination were included in the study. Culture and mNGS were performed simultaneously for all patients. Clinical data were retrieved for analysis.
    RESULTS: A total of 78 patients were enrolled, with 40 in the talaromycosis group and 38 in the suspected-talaromycosis group. In the talaromycosis group, mNGS showed a higher positivity rate(40/40, 100.0%) compared to culture(34/40, 85.0%)(P = 0.111). All patients in the suspected-talaromycosis group tested negative via culture, while mNGS yielded positive results. The T. marneffei reads in the talaromycosis group were significantly higher than in the suspected-talaromycosis group (4399 vs. 28, P < 0.001). In the suspected-talaromycosis group, of the four patients with low reads who did not receive antifungal therapy, one died and one lung lesion progressed; most patients(31/34, 91.2%) recovered after receiving appropriate antifungal therapy.
    CONCLUSIONS: mNGS proves to be a rapid and highly sensitive method for detecting T. marneffei. Higher reads of T. marneffei correspond to a higher likelihood of infection. However, cases with low reads necessitate a comprehensive approach, integrating clinical manifestations, laboratory tests, and imaging examinations to confirm T. marneffei infection.
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  • 文章类型: Journal Article
    本研究旨在探讨宏基因组下一代测序(mNGS)在肺弥漫性渗出性病变中的临床应用价值。
    从2014年1月1日至2021年11月31日,福建省立医院收治的136例胸部影像学表现为肺弥漫性渗出性病变的患者纳入研究;其中,77例患者行mNGS病原体检测。根据病原体检测结果和临床诊断,患者分为感染组(IG)和非感染组(NIG).比较了mNGS技术和传统培养方法的诊断效能。同时,59名临床鉴定为具有感染性肺弥漫性渗出性病变但未接受mNGS测试的患者被指定为非NGS感染组(非IG)。对IG和非IG患者进行了回顾性队列研究,30天全因死亡率终点用于随访。
    与常规培养方法相比,mNGS的灵敏度提高了约35%(80.0%vs45.5%,P<0.001),特异性无显著差异(77.3%vs95.5%,P=0.185)。在接触抗生素的情况下,mNGS检测的阳性率明显高于传统培养方法,表明mNGS受抗生素暴露的影响较小(P<0.05)。30天内,IG与非IG患者的全因死亡率分别为14.55%和37.29%,分别为(P<0.05)。在进行COX回归分析以调整混杂因素后,分析显示,CURB-65评分≥3分(HR=3.348,P=0.001)和存在心血管疾病(HR=2.473,P=0.026)是这些患者的独立危险因素.相反,mNGS检测(HR=0.368,P=0.017)是一个独立的保护因素。
    mNGS技术可以更轻松地查明肺部弥漫性感染性渗出性病变的原因,而不会受到抗生素的太多干扰,帮助医生尽早发现和诊断这些问题,从而在帮助他们为患者决定最佳治疗方法方面发挥关键作用。这样的结论可能有偏见,因为缺乏血清学检测和PCR等其他常规诊断技术的完整结果,传统方法的性能可能被低估。
    UNASSIGNED: This study aims to investigate the clinical application value of Metagenome Next-Generation Sequencing (mNGS) for pulmonary diffuse exudative lesions.
    UNASSIGNED: From January 1, 2014, to November 31, 2021, 136 cases with chest radiologic presentations of pulmonary diffuse exudative lesions admitted to Fujian Provincial Hospital were included in the study; of those, 77 patients underwent mNGS pathogen detection. Based on the pathogen detection outcomes and clinical diagnoses, patients were categorized into an infection group (IG) and a non-infection group (NIG). A comparison was made between the diagnostic efficacy of the mNGS technique and traditional culture methods. Meanwhile, 59 patients clinically identified as having infectious pulmonary diffuse exudative lesions but who did not receive mNGS testing were designated as the non-NGS infection group (non-IG). A retrospective cohort study was conducted on patients in both the IG and non-IG, with a 30-day all-cause mortality endpoint used for follow-up.
    UNASSIGNED: When compared to conventional culture methods, mNGS demonstrated an approximate 35% increase in sensitivity (80.0% vs 45.5%, P<0.001), without significant disparity in specificity (77.3% vs 95.5%, P=0.185). Under antibiotic exposure, the positivity rate detected by mNGS was notably higher than that by traditional culture methods, indicating that mNGS is less affected by exposure to antibiotics (P<0.05). Within 30 days, the all-cause mortality rate for patients in the IG versus the non-IG was 14.55% and 37.29%, respectively (P<0.05). Following a COX regression analysis to adjust for confounding factors, the analysis revealed that a CURB-65 score ≥3 points (HR=3.348, P=0.001) and existing cardiovascular disease (HR=2.473, P=0.026) were independent risk factors for these patients. Conversely, mNGS testing (HR=0.368, P=0.017) proved to be an independent protective factor.
    UNASSIGNED: mNGS technology makes it easier to pinpoint the cause of pulmonary diffuse infectious exudative lesions without much interference from antibiotics, helping doctors spot and diagnose these issues early on, thereby playing a key role in helping them decide the best treatment approach for patients. Such conclusions may have a bias, as the performance of traditional methods might be underestimated due to the absence of complete results from other conventional diagnostic techniques like serological testing and PCR.
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  • 文章类型: Journal Article
    背景:本研究旨在评估宏基因组下一代测序(mNGS)技术在关节假体周围感染(PJI)中鉴定病原体的应用。
    方法:对2020年4月至2023年7月期间怀疑患有PJI的65例患者进行了回顾性分析。根据2018年国际共识会议标准,将患者分为PJI(46例)和非PJI(19例)组。收集临床数据,并进行常规细菌培养和mNGS。对比分析了两种方法的诊断性能。
    结果:mNGS的灵敏度为89.13%,特异性为94.74%,阳性预测值为97.62%,阴性预测值为78.26%,总体诊断准确率为90.77%。与微生物培养相比,mNGS表现出优异的诊断灵敏度,同时保持相似的特异性。使用mNGS成功鉴定了48种病原体,凝固酶阴性葡萄球菌,链球菌,金黄色葡萄球菌,粉刺杆菌是最常见的传染因子。值得注意的是,mNGS用于鉴定14个培养阴性PJI样品中的17种潜在病原体,突出了它检测罕见传染因子的能力,包括粉刺杆菌(n=5),绝热颗粒菌(n=1),结核分枝杆菌复合体(n=1),和伯氏柯西拉(n=1),其中,常规培养方法检测不到。然而,mNGS在4例培养阳性的PJI患者中未能检测到病原体,表明其局限性。在46名PJI患者中,27具有阳性培养和mNGS结果。mNGS的结果与6例PJI患者的属水平和18例患者的属水平的培养结果一致。此外,本研究显示,窦道组金黄色葡萄球菌的比例(45.45%)明显高于非窦道组(14.29%),表明该病原体与PJI中的窦道形成相关(P=0.03)。此外,窦道组(27.27%)与非窦道组(33.33%)之间的多微生物感染发生率差异无统计学意义(P=0.37)。
    结论:除传统培养方法外,宏基因组下一代测序还可以作为一种有价值的筛选工具,通过优化培养策略提高诊断准确性。
    BACKGROUND: This study aimed to evaluate the application of metagenomic next-generation sequencing (mNGS) technology to identify pathogens in periprosthetic joint infection (PJI).
    METHODS: A retrospective analysis was conducted on 65 patients suspected of having PJI between April 2020 and July 2023. The patients were categorized into PJI (46 patients) and non-PJI (19 patients) groups based on the 2018 International Consensus Meeting criteria. Clinical data were collected, and both conventional bacterial culture and mNGS were performed. The diagnostic performance of the two methods was compared and analyzed.
    RESULTS: mNGS exhibited a sensitivity of 89.13%, a specificity of 94.74%, a positive predictive value of 97.62%, a negative predictive value of 78.26%, and an overall diagnostic accuracy of 90.77%. Compared to microbial culture, mNGS demonstrated superior diagnostic sensitivity while maintaining similar specificity. A total of 48 pathogens were successfully identified using mNGS, with Coagulase-negative staphylococci, Streptococci, Staphylococcus aureus, and Cutibacterium acnes being the most common infectious agents. Notably, mNGS was used to identify 17 potential pathogens in 14 culture-negative PJI samples, highlighting its ability to detect rare infectious agents, including Cutibacterium acnes (n = 5), Granulicatella adiacens (n = 1), Mycobacterium tuberculosis complex (n = 1), and Coxiella burnetii (n = 1), among others, which are not detectable by routine culture methods. However, mNGS failed to detect the pathogen in 4 culture-positive PJI patients, indicating its limitations. Among the 46 PJI patients, 27 had positive culture and mNGS results. The results of mNGS were concordant with those of culture at the genus level in 6 patients with PJI and at the species level in 18 patients. Furthermore, the present study revealed a significantly greater proportion of Staphylococcus aureus in the sinus tract group (45.45%) than in the non-sinus tract group (14.29%), indicating the association of this pathogen with sinus formation in PJI (P = 0.03). Additionally, there was no significant difference in the occurrence of polymicrobial infections between the sinus tract group (27.27%) and the non-sinus tract group (33.33%) (P = 0.37).
    CONCLUSIONS: Metagenomic next-generation sequencing can serve as a valuable screening tool in addition to traditional culture methods to improve diagnostic accuracy through optimized culture strategies.
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  • 文章类型: Journal Article
    研究宏基因组下一代测序(mNGS)在非人类免疫缺陷病毒(HIV)感染患者中诊断吉罗韦西肺孢子虫肺炎(PJP)的价值。
    在这项回顾性研究中,选择2022年8月至2024年12月非HIV感染的PJP患者和非PJP诊断患者作为受试者.分析了支气管肺泡灌洗液(BALF)中肺孢子虫(PJ)和其他共同病原体的存在,以及NGS的诊断效能,将PJP中的聚合酶链反应(PCR)和血清1,3-β-D-葡聚糖(BDG)与临床复合诊断的参考标准进行比较。
    招募了89名非HIV感染者,以呼吸困难为主要症状(69.66%),以实体恶性肿瘤为最常见的基础疾病(20.22%)。以临床综合诊断为参考标准,灵敏度,特异性,mNGS的阴性预测值和阳性预测值均高于PCR和血清BDG。在42名非HIV感染的PJP患者中,接受了mNGS和常规病原体检测的BALF,6例单纯PJ感染,36例合并PJ感染。混合感染中mNGS的检出率明显高于常规病原体检测(85.71vs61.70%,P=0.012)。使用mNGS在BALF中总共检测到127种病原体,其中真菌检出率最高(46.46%)。真菌,检测到的病毒和细菌主要是肺孢子虫,人γ疱疹病毒4型和鲍曼不动杆菌。
    mNGS在诊断非HIV感染的PJP患者中非常有效,并且在检测共同病原体方面表现出理想的性能。此外,对临床诊断和指导针对性抗感染药物治疗具有一定的价值。
    UNASSIGNED: To investigate the value of metagenomic Next-Generation Sequencing (mNGS) in diagnosing Pneumocystis jirovecii pneumonia (PJP) in non-human immunodeficiency virus (HIV)-infected patients.
    UNASSIGNED: In this retrospective study, non-HIV-infected patients with PJP and those diagnosed with non-PJP from August 2022 to December 2024 were selected as subjects. The presence of Pneumocystis jirovecii (PJ) and other co-pathogens in bronchoalveolar lavage fluid (BALF) was analyzed, and the diagnostic efficacy of NGS, polymerase chain reaction (PCR) and serum 1,3-β-D-glucan (BDG) in PJP was compared with the reference standard of clinical compound diagnosis.
    UNASSIGNED: Eighty-nine non-HIV-infected patients were recruited, with dyspnea as the primary symptom (69.66%) and solid malignant tumor as the most common underlying disease (20.22%). Taking clinical compound diagnosis as the reference standard, the sensitivity, specificity, negative predictive value and positive predictive value of mNGS were higher than those detected by PCR and serum BDG. Among 42 non-HIV-infected patients with PJP who underwent mNGS and conventional pathogen detection of BALF, 6 had simple PJ infection and 36 had combined PJ infection. The detection rate of mNGS in mixed infections was significantly higher than that of conventional pathogen detection (85.71 vs 61.70%, P = 0.012). A total of 127 pathogens were detected in BALF using mNGS, among which fungi had the highest detection rate (46.46%). The fungi, viruses and bacteria detected were mainly Pneumocystis jirovecii, human gammaherpesvirus 4 and Acinetobacter baumannii.
    UNASSIGNED: mNGS is highly effective in diagnosing non-HIV-infected patients with PJP and exhibits ideal performance in the detection of co-pathogens. In addition, it has certain value for clinical diagnosis and guidance of targeted anti-infective drug treatment.
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  • 文章类型: Journal Article
    背景:下一代测序(NGS)可能有助于病原体的鉴定。然而,用于脑脊液(CSF)检测的最佳方法尚不清楚,评估不同NGS工作流程在颅内感染诊断中的应用的研究有限。
    方法:在这个多中心中,前瞻性观察性队列研究,我们描述了病原体靶向NGS(ptNGS)和宏基因组NGS(mNGS)的诊断功效,用于传染性脑膜炎/脑炎(M/E)。
    结果:总计,纳入了在四家三级医院诊断为临床可疑M/E的152例患者;同时使用ptNGS和mNGS进行CSF病原体检测。在89例确诊为明确感染性M/E的患者中,57和39例患者通过ptNGS和mNGS进行了因果微生物检测,分别。ptNGS的总体准确率为65.1%,正百分比协议(PPA)为64%,负百分比协议(NPA)为66.7%;mNGS的总体准确性为47.4%,差异分析后PPA为43.8%,NPA为52.4%。两种检测方法对PPA的检测效率(灵敏度)和病原体检测的总体准确性均存在显着差异(P<0.05)。
    结论:NGS测试提供了除常规微生物测试之外的新信息。对于感染性M/E的CSF中的常见致病病原体检测,ptNGS似乎比mNGS具有更优越的性能。
    BACKGROUND: Next-generation sequencing (NGS) might aid in the identification of causal pathogens. However, the optimal approaches applied to cerebrospinal fluid (CSF) for detection are unclear, and studies evaluating the application of different NGS workflows for the diagnosis of intracranial infections are limited.
    METHODS: In this multicenter, prospective observational cohort study, we described the diagnostic efficacy of pathogen-targeted NGS (ptNGS) and metagenomic NGS (mNGS) compared to that of composite microbiologic assays, for infectious meningitis/encephalitis (M/E).
    RESULTS: In total, 152 patients diagnosed with clinically suspected M/E at four tertiary hospitals were enrolled; ptNGS and mNGS were used in parallel for pathogen detection in CSF. Among the 89 patients who were diagnosed with definite infectious M/E, 57 and 39 patients had causal microbial detection via ptNGS and mNGS, respectively. The overall accuracy of ptNGS was 65.1%, with a positive percent agreement (PPA) of 64% and a negative percent agreement (NPA) of 66.7%; and the overall accuracy of mNGS was 47.4%, with a PPA of 43.8% and an NPA of 52.4% after discrepancy analysis. There was a significant difference in the detection efficiency between these two methods both for PPA (sensitivity) and overall accuracy for pathogen detection (P < 0.05).
    CONCLUSIONS: NGS tests have provided new information in addition to conventional microbiologic tests. ptNGS seems to have superior performance over mNGS for common causative pathogen detection in CSF for infectious M/E.
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  • 文章类型: Journal Article
    本研究旨在描述和比较流行病学,人口统计学,临床,实验室和放射学特征以及并发症,治疗,以及这些患者的结果。
    我们回顾性调查了福建8所三甲医院的鹦鹉感染(鹦鹉病)患者的临床资料。使用宏基因组下一代测序(mNGS)鉴定所有包括的患者的临床样品中的鹦鹉。
    共有74例患者(39例严重/35例非严重)被诊断为鹦鹉病,其中25人(33.8%)有家禽接触史。常见症状包括高烧(98%[37/74]),疲劳(52.7%[39/74]),和呼吸困难(51.4%[38/74])。影像学的常见表现包括巩固(89.2%),胸腔积液(77.0%),和空气支气管图(66.2%)。常见的并发症包括急性呼吸窘迫综合征(55.4%[41/74]),I型呼吸衰竭(52.7%[39/74]),急性肝损伤(41.9%[31/74]),继发感染(27.0%[20/74])。住院死亡率为8.11%(6/74)。
    C.鹦鹉螺感染是导致CAP被低估的原因。对于有家禽和鸟类接触史的SCAP患者,鼓励及时送检标本进行mNGS检测。C.鹦鹉感染可导致严重,多系统参与,和几个并发症。mNGS有助于鹦鹉感染的及时诊断。
    UNASSIGNED: This study aimed to describe and compare the epidemiological, demographic, clinical, laboratory and radiological characteristics as well as the complications, treatments, and outcomes of these patients.
    UNASSIGNED: We retrospectively investigated clinical data of patients with C. psittaci infection (psittacosis) in eight Grade IIIA hospitals of Fujian. Metagenomic next-generation sequencing (mNGS) was used identify C. psittaci in clinical samples of all included patients.
    UNASSIGNED: A total of 74 patients (39 severe/35 non-severe) was diagnosed with psittacosis, 25 (33.8%) of whom had history of poultry exposure. Common symptoms included high fever (98% [37/74]), fatigue (52.7% [39/74]), and dyspnea (51.4% [38/74]). Common manifestations in imaging included consolidation (89.2%), pleural effusion (77.0%), and air bronchogram (66.2%). Common complications included acute respiratory distress syndrome (55.4% [41/74]), type I respiratory failure (52.7% [39/74]), acute liver injury (41.9% [31/74]), and secondary infection (27.0% [20/74]). The in-hospital mortality rate was 8.11% (6/74).
    UNASSIGNED: C. psittaci infection is represents an underestimated cause of CAP. For SCAP patients with poultry and bird contact history, specimens were encouraged to be sended for mNGS test in time. C. psittaci infection can lead to severe, multiple system involvement, and several complications. mNGS facilitate timely diagnosis of C. psittaci infection.
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  • 文章类型: Multicenter Study
    背景:在经过彻底的诊断检查后,高达45%的高热返回旅客仍未确诊,甚至在转诊中心.尽管宏基因组下一代测序(mNGS)已成为一种有前途的工具,证明其在输入性发热中有用的证据非常有限。
    方法:2017年11月至2019年11月,在三家转诊诊所前瞻性招募了因发烧而返回的旅行者。对患有急性未分化发热疾病(AUFI)的参与者的血清样品进行了针对病毒检测优化的无偏mNGS,并将结果与通过参考诊断方法(RDM)获得的结果进行了比较。
    结果:在507名返回的发热旅行者中,433(85.4%)呈现AUFI。登革热病毒(n=86)和疟原虫。(n=83)是发烧的最常见原因。103/433(23.8%)AUFI在随访结束时仍未诊断。mNGS在196/433(38.7%)AUFI中揭示了潜在的致病微生物。mNGS鉴定在发热持续时间较短的患者中更为常见(≤5天的42.3%与>5天内28.7%,p=0.005)。在25/103(24.2%)未诊断的AUFI和5/23(21.7%)患有严重未诊断的AUFI的旅行者中发现了发烧的潜在原因。错过的严重病因包括8个细菌鉴定和1个B19细小病毒和曲霉属的共感染。额外的鉴定表明29/316(9.2%)的AUFI旅客可能合并感染,在严重AUFI的11/128(8.6%)旅客中,通过RDM接受诊断的人。在严重AUFI中检测到的大多数常见共感染是由革兰氏阴性菌引起的。血清mNGS无法检测到RDM获得的>50%的感染性诊断,并且还获得了607个非致病性鉴定。
    结论:血清mNGS除了参考诊断技术外,对于未诊断出AUFI或严重疾病的特定旅行者来说,可以成为有价值的诊断工具。尤其是在症状出现的最初几天。然而,mNGS结果解释提出了巨大的挑战。需要使用针对非病毒试剂定制的不同样品类型和方案来评估mNGS的性能的进一步研究。
    BACKGROUND: Up to 45% of febrile returning travellers remain undiagnosed after a thorough diagnostic work-up, even at referral centres. Although metagenomic next-generation sequencing (mNGS) has emerged as a promising tool, evidence of its usefulness in imported fever is very limited.
    METHODS: Travellers returning with fever were prospectively recruited in three referral clinics from November 2017 to November 2019. Unbiased mNGS optimised for virus detection was performed on serum samples of participants with acute undifferentiated febrile illness (AUFI), and results were compared to those obtained by reference diagnostic methods (RDM).
    RESULTS: Among 507 returned febrile travellers, 433(85.4%) presented with AUFI. Dengue virus (n = 86) and Plasmodium spp. (n = 83) were the most common causes of fever. 103/433(23.8%) AUFI remained undiagnosed at the end of the follow-up.Metagenomic next-generation sequencing unveiled potentially pathogenic microorganisms in 196/433(38.7%) AUFI. mNGS identifications were more common in patients with a shorter duration of fever (42.3% in ≤5 days vs 28.7% in >5 days, P = 0.005). Potential causes of fever were revealed in 25/103(24.2%) undiagnosed AUFI and 5/23(21.7%) travellers with severe undiagnosed AUFI. Missed severe aetiologies included eight bacterial identifications and one co-infection of B19 parvovirus and Aspergillus spp.Additional identifications indicating possible co-infections occurred in 29/316(9.2%) travellers with AUFI, and in 11/128(8.6%) travellers with severe AUFI, who had received a diagnosis through RDM. The most common co-infections detected in severe AUFI were caused by Gram-negative bacteria. Serum mNGS was unable to detect >50% of infectious diagnoses achieved by RDM and also yielded 607 non-pathogenic identifications.
    CONCLUSIONS: mNGS of serum can be a valuable diagnostic tool for selected travellers with undiagnosed AUFI or severe disease in addition to reference diagnostic techniques, especially during the first days of symptoms. Nevertheless, mNGS results interpretation presents a great challenge. Further studies evaluating the performance of mNGS using different sample types and protocols tailored to non-viral agents are needed.
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  • 文章类型: Journal Article
    本研究的目的是比较宏基因组下一代测序(mNGS)与慢性感染和急性感染的常规培养方法(CM)。
    我们回顾性分析了2017年至2022年三所医院收治的88例急性感染患者和105例慢性感染患者的支气管肺泡灌洗液(BALF)。
    结果表明,mNGS的敏感性和特异性均高于CM。在两个急性感染组中,mNGS阳性组改变抗生素治疗的患者人数均大于mNGS阴性组的患者(60.5vs.28.0%,P=0.0022)和慢性感染组(46.2vs.22.6%,P=0.01112)。高温(OR:2.02,95%CI:1.18-3.70,P:0.015),C反应蛋白(CRP)(OR:15,95%CI:2.74-280.69,P:0.011),中性粒细胞计数(OR:3.09,95%CI:1.19-8.43,P:0.023),淋巴细胞计数水平低(OR:3.43,95%CI:1.26-10.21,P:0.020)可能导致急性感染组mNGS结果阳性,而在慢性感染组中没有发现预测阳性结果的重要因素组。
    mNGS可以为感染性疾病的抗生素策略提供有用的指导,并且可能对急性感染的诊断和治疗更有价值。慢性感染。
    UNASSIGNED: The aim of this study is to compare the diagnostic value of metagenomic next-generation sequencing (mNGS) vs. conventional culture methods (CM) in chronic infection and acute infection.
    UNASSIGNED: We retrospectively analyzed the bronchoalveolar lavage fluid (BALF) of 88 patients with acute infection and 105 patients with chronic infection admitted to three hospitals from 2017 to 2022.
    UNASSIGNED: The results showed that the sensitivity and specificity of mNGS were higher than those of CM. The number of patients who changed the antibiotic treatment in the mNGS positive group was larger than that of patients in the mNGS negative group in both the acute infection group (60.5 vs. 28.0%, P = 0.0022) and chronic infection group (46.2 vs. 22.6%, P = 0.01112). High levels of temperature (OR: 2.02, 95% CI: 1.18-3.70, P: 0.015), C-reactive protein (CRP) (OR: 15, 95% CI: 2.74-280.69, P: 0.011), neutrophil count (OR: 3.09, 95% CI: 1.19-8.43, P: 0.023), and low levels of lymphocyte count (OR: 3.43, 95% CI:1.26-10.21, P: 0.020) may lead to positive mNGS results in the acute infection group while no significant factor was identified to predict positive results in the chronic infection group.
    UNASSIGNED: mNGS could provide useful guidance on antibiotic strategies in infectious diseases and may be more valuable for the diagnosis and treatment of acute infection vs. chronic infection.
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