emergomycosis

白纹真菌病
  • 文章类型: Journal Article
    在由两部分组成的继续医学教育系列的第一部分中,流行病学,临床特征,和真菌皮肤被忽视热带病(NTDs)的诊断方法,其中包括Eumycetoma,成色真菌病,副角菌病,孢子丝菌病,真菌病,塔拉真菌病,和大孢子菌病,被审查。这些感染,其中一些被世界卫生组织(世卫组织)正式指定为NTD,在全球范围内引起大量发病率和污名,并且由于与气候变化相关的地理扩展的潜力而受到越来越多的关注。在全球旅行和免疫抑制的背景下,国内发病率可能会增加。美国皮肤科医生可能在早期发现和开始适当治疗方面发挥核心作用,导致发病率和死亡率下降。
    In this part 1 of a 2-part continuing medical education series, the epidemiology, clinical features, and diagnostic methods for fungal skin neglected tropical diseases (NTDs), which include eumycetoma, chromoblastomycosis, paracoccidioidomycosis, sporotrichosis, emergomycosis, talaromycosis, and lobomycosis, are reviewed. These infections, several of which are officially designated as NTDs by the World Health Organization (WHO), cause substantial morbidity and stigma worldwide and are receiving increased attention due to the potential for climate change-related geographic expansion. Domestic incidence may be increasing in the setting of global travel and immunosuppression. United States dermatologists may play a central role in early detection and initiation of appropriate treatment, leading to decreased morbidity and mortality.
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  • 文章类型: Journal Article
    在由两部分组成的继续医学教育系列的第二部分中,管理层,结果,和真菌皮肤被忽视的热带病(NTDs)的发病率,包括Eumycetoma,成色真菌病,副角菌病,孢子丝菌病,真菌病,塔拉真菌病,对叶真菌病进行了综述。虽然在资源有限的环境中,真菌皮肤NTD与贫困有关,在美国,它们更经常与免疫抑制和全球移民有关。这些感染有很高的发病率负担,包括毁容,身体残疾,共感染,恶性转化,心理健康问题,和财务影响。对于大多数真菌皮肤NTDs,管理困难,治愈率低。皮肤科医生在疾病早期启动适当治疗以改善患者预后方面发挥着核心作用。
    In this part 2 of a 2-part continuing medical education series, the management, outcomes, and morbidities for fungal skin neglected tropical diseases (NTDs), including eumycetoma, chromoblastomycosis, paracoccidioidomycosis, sporotrichosis, emergomycosis, talaromycosis, and lobomycosis are reviewed. While fungal skin NTDs are associated with poverty in resource-limited settings, they are more often associated with immunosuppression and global migration in the United States. These infections have a high morbidity burden, including disfigurement, physical disability, coinfection, malignant transformation, mental health issues, and financial impact. For most fungal skin NTDs, management is difficult and associated with low cure rates. Dermatologists play a central role in initiating appropriate treatment early in disease course in order to improve patient outcomes.
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  • 文章类型: Journal Article
    我们进行了体外抗真菌药敏试验manogepix对78种非洲产卵酵母的酵母期,2巴斯德氏菌,根据临床和实验室标准研究所的建议,使用参考肉汤微量稀释法分离5株胚芽菌。所有三种病原体的最低抑制浓度均低于0.0005至0.008mg/L。Manogepix应在动物模型中进行研究,并可能在未来的地方性真菌病人体临床试验中进行研究。
    We performed in vitro antifungal susceptibility testing of manogepix against the yeast phase of 78 Emergomyces africanus, 2 Emergomyces pasteurianus, and 5 Blastomyces emzantsi isolates using a reference broth microdilution method following Clinical and Laboratory Standards Institute recommendations. All three pathogens had low minimum inhibitory concentrations ranging from <0.0005 to 0.008 mg/L. Manogepix should be investigated in animal models and potentially in future human clinical trials for endemic mycoses.
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  • 文章类型: Journal Article
    Emergomycosis是由Emergomes物种引起的地方性真菌病。由于该试剂引起的感染已在全球范围内报道。因此,本系统综述对胚胎属感染进行了研究,以研究疾病流行病学,潜在的疾病和危险因素,病原体,治疗和结果。MEDLINE,Scopus,Embase,从1990年1月到2022年10月,使用适当的关键词系统地搜索了WebofScience数据库。共纳入77例毛菌病病例分析。在患有人类免疫缺陷病毒(HIV)感染的患者(n=61,79.2%)和患有或不患有其他合并症的未感染HIV的患者(n=16,20.8%)中最常见病。在HIV感染患者中,潜在的疾病和危险因素显著相关的是CD4+T细胞计数小于100细胞/mm3(n=55,90.2%),贫血(n=30,49.2%),和血小板减少症(n=17,27.9%),而在未感染艾滋病毒的患者中,用免疫抑制药物治疗(n=10,62.5%),肾脏疾病(n=8,50%),移植受者(n=6,37.5%),糖尿病(n=4,25%)是与emergomycosis相关的重要危险因素。非洲胚(n=55,71.4%)是最常见的病原体,其次是E.pasteurianus(n=9,11.7%)和E.canadensis(n=5,6.5%)。最常分离自HIV感染患者(n=54,98.2%),而E.pasteurianus在未感染HIV的患者中最常见(n=5,55.6%)。整个队列的全因死亡率为42.9%。在HIV感染患者(n=28,36.4%)和未感染HIV的患者(n=5,6.5%)之间没有观察到死亡率的显着差异。总之,随着全球除艾滋病毒感染外,免疫抑制人口的增加,在未来可能会增加的病例负担。因此,临床医生和真菌学家应保持警惕,并在临床上怀疑是否有真菌病,这有助于早期诊断和开始抗真菌治疗,以防止疾病死亡。
    Emergomycosis is an endemic mycosis caused by the Emergomyces species. Infections due to this agent have been reported globally. Hence, the present systematic review on Emergomyces infections was conducted to study the disease epidemiology, underlying diseases and risk factors, causative agents, and treatment and outcome. The MEDLINE, Scopus, Embase, and Web of Science databases were searched systematically with appropriate keywords from January 1990 to October 2022. A total of 77 cases of emergomycosis were included in the analysis. Emergomycosis was most commonly seen in patients with human immunodeficiency virus (HIV) infection (n = 61, 79.2%) and HIV-uninfected patients with or without other comorbidities (n = 16, 20.8%). The underlying disease and risk factors significantly associated with emergomycosis in the HIV-infected patients were CD4+ T-cell counts less than 100 cells/mm3 (n = 55, 90.2%), anaemia (n = 30, 49.2%), and thrombocytopenia (n = 17, 27.9%), whereas in the HIV-uninfected patients, treatment with immunosuppressive drugs (n = 10, 62.5%), renal disease (n = 8, 50%), transplant recipients (n = 6, 37.5%), and diabetes mellitus (n = 4, 25%) were the significant risk factors associated with emergomycosis. Emergomyces africanus (n = 55, 71.4%) is the most common causative agent, followed by E. pasteurianus (n = 9, 11.7%) and E. canadensis (n = 5, 6.5%). E. africanus was most often isolated from HIV-infected patients (n = 54, 98.2%), whereas E. pasteurianus was most common in HIV-uninfected patients (n = 5, 55.6%). The all-cause mortality rate of the total cohort is 42.9%. No significant variation in the mortality rate is observed between the HIV-infected patients (n = 28, 36.4%) and the HIV-uninfected patients (n = 5, 6.5%). In conclusion, with an increase in the immunosuppressed population across the globe in addition to HIV infection, the case burden of emergomycosis may increase in the future. Hence, clinicians and mycologists should be vigilant and clinically suspicious of emergomycosis, which helps in early diagnosis and initiation of antifungal treatment to prevent disease mortality.
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  • 文章类型: Journal Article
    白纹菌病是一种新兴的致命传染病,主要由鲜为人知的空气传播病原体非洲白纹菌引起,这可能会导致临床管理挑战,尤其是在晚期HIV患者中。这篇小型评论描述了Es。非洲是非洲的主要原因,并考虑了造成这种感染管理困难的因素。在CD4淋巴细胞计数较低的HIV阳性人群中常见,估计死亡率为50%。感染表现为空气传播,肺部和肺外表现导致皮肤病变。然而,Es的发病机制。非洲仍然知之甚少。由于缺乏明确的诊断和治疗指南,感染的管理很复杂。专业知识有限,可怜的研究经费,缺乏意识和国家监测被认为会影响感染的识别和优先次序。这些因素最终可能会将青霉病指定为“被忽视的感染状态”,即使它被怀疑在比以前公认的更多的非洲国家流行。提高认识和综合和有针对性的战略,如动员人力在临床真菌学是至关重要的管理在非洲及其他地区的紧急真菌病。
    Emergomycosis is an emerging deadly infectious disease caused primarily by a little-known airborne pathogen Emergomyces africanus, which can cause clinical management challenge especially in patients with advanced HIV disease. This minireview describes Es. africanus as the main cause of emergomycosis in Africa as well as considers contributing factors to the difficulties encountered in managing this infection. Emergomycosis is common in HIV-positive persons with low CD4 lymphocyte count and has an estimated fatality of 50%. The infection exhibits airborne transmission with pulmonary and extrapulmonary manifestations leading to skin lesions. However, the pathogenesis of Es. africanus is still poorly understood. The management of the infection is complicated due to lack of defined diagnostic and therapeutic guidelines. Limited expertise, poor research funding, and lack of awareness and national surveillance are thought to impact the recognition and prioritisation of the infection. These factors may ultimately assign emergomycosis a \'neglected infection status\' even as it is suspected to be prevalent in more African countries than previously recognised. Increased awareness and integrated and targeted strategies such as mobilising manpower in clinical mycology are of paramount importance in managing emergomycosis in Africa and beyond.
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  • 文章类型: Journal Article
    侵袭性真菌病(IFD)在资源有限的环境中备受关注,尤其是在非洲,由于IFD的诊断设备不可用,从而使明确的诊断具有挑战性。IFD具有与更频繁的疾病重叠的非特异性系统性表现,如肺结核,艾滋病毒,以及与HIV相关的机会性感染和恶性肿瘤。因此,IFD通常未被诊断或误诊。我们批判性地审查了有关非洲IFD的现有文献,以更好地了解其流行病学,疾病负担,以指导未来的研究和干预。隐球菌病是非洲遇到最多的IFD,占撒哈拉以南非洲地区艾滋病毒相关死亡的大多数。侵袭性曲霉病,虽然有些未被诊断和/或误诊为结核病,越来越多的报道对艾滋病毒感染者有类似的偏好。最近的流行病学研究也报道了更多的组织胞浆菌病病例,特别是来自西非,在推定结核病患者和艾滋病毒感染者中显示出很高的患病率。肺囊虫肺炎的负担已显著减少,这可能是由于非洲艾滋病毒感染者接受抗逆转录病毒疗法的增加,和全球。毛霉菌病,塔拉真菌病,真菌病,芽生菌病,和球菌病也有报道,但文献研究很少。正如其他地区报道的那样,非洲对大多数可用抗真菌药物的耐药性的出现仍然引起了极大的关注。非洲的IFD比看起来更常见,并且对发病率和死亡率有很大贡献。需要巨大的投资来推动意识和真菌相关研究,特别是在诊断和抗真菌治疗方面。
    Invasive fungal diseases (IFDs) are of huge concern in resource-limited settings, particularly in Africa, due to the unavailability of diagnostic armamentarium for IFDs, thus making definitive diagnosis challenging. IFDs have non-specific systemic manifestations overlapping with more frequent illnesses, such as tuberculosis, HIV, and HIV-related opportunistic infections and malignancies. Consequently, IFDs are often undiagnosed or misdiagnosed. We critically reviewed the available literature on IFDs in Africa to provide a better understanding of their epidemiology, disease burden to guide future research and interventions. Cryptococcosis is the most encountered IFD in Africa, accounting for most of the HIV-related deaths in sub-Saharan Africa. Invasive aspergillosis, though somewhat underdiagnosed and/or misdiagnosed as tuberculosis, is increasingly being reported with a similar predilection towards people living with HIV. More cases of histoplasmosis are also being reported with recent epidemiological studies, particularly from Western Africa, showing high prevalence rates amongst presumptive tuberculosis patients and patients living with HIV. The burden of pneumocystis pneumonia has reduced significantly probably due to increased uptake of anti-retroviral therapy among people living with HIV both in Africa, and globally. Mucormycosis, talaromycosis, emergomycosis, blastomycosis, and coccidiomycosis have also been reported but with very few studies from the literature. The emergence of resistance to most of the available antifungal drugs in Africa is yet of huge concern as reported in other regions. IFDs in Africa is much more common than it appears and contributes significantly to morbidity and mortality. Huge investment is needed to drive awareness and fungi related research especially in diagnostics and antifungal therapy.
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  • 文章类型: Journal Article
    地方性真菌病芽生菌病,球孢子菌病,组织胞浆菌病,副角菌病,隐球菌病,孢子丝菌病,塔拉真菌病,非肉芽肿病,和真菌病主要是由地理上有限的热二形真菌引起的(隐球菌病除外),他们的诊断可能具有挑战性。地方性真菌病诊断中涉及的通常实验室方法包括显微镜检查和生物样品的培养;然而,血清学,组织病理学,在过去的几年中,已经实施了分子技术来诊断这些真菌病,因为它们的病原体的恢复和鉴定耗时且缺乏敏感性。在这次审查中,我们专注于与抗体和抗原检测相关的免疫诊断方法,因为它们的证据是推定诊断,在一些真菌病中,比如隐球菌病,这是明确的诊断。
    The endemic mycoses blastomycosis, coccidioidomycosis, histoplasmosis, paracoccidioidomycosis, cryptococcosis, sporotrichosis, talaromycosis, adiaspiromycosis, and emergomycosis are mostly caused by geographically limited thermally dimorphic fungi (except for cryptococcosis), and their diagnoses can be challenging. Usual laboratory methods involved in endemic mycoses diagnosis include microscopic examination and culture of biological samples; however, serologic, histopathologic, and molecular techniques have been implemented in the last few years for the diagnosis of these mycoses since the recovery and identification of their etiologic agents is time-consuming and lacks in sensitivity. In this review, we focus on the immunologic diagnostic methods related to antibody and antigen detection since their evidence is presumptive diagnosis, and in some mycoses, such as cryptococcosis, it is definitive diagnosis.
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  • 文章类型: Journal Article
    审查的目的在这篇审查中,我们从临床角度提供了一个概述,并讨论了分类和分类的病原体,流行病学,感染的病理生理学和发病机制,免疫学,临床表现,实验室培养和诊断,分子表征,治疗和预后。最近的研究结果虽然巴斯德氏菌是地理上分布最广泛的物种,非洲雏菊是南部非洲的地方病,主要在晚期人类免疫缺陷病毒(HIV)疾病患者中引起皮肤累及的播散性疾病。总结出毛菌病,一种传播的临床疾病,是由于感染了Emergomyces属的双态真菌而引起的,主要发生在免疫功能低下的患者中。需要进一步了解病理生理学,真菌病的诊断和治疗。
    Purpose of Review In this review, we provide an overview of emergomycosis from a clinical perspective and discuss the taxonomy and classification of the pathogens, epidemiology, pathophysiology of infection and mechanisms of pathogenesis, immunology, clinical manifestations, laboratory culture and diagnosis, molecular characterisation, therapy and prognosis. Recent Findings While Emergomyces pasteurianus is the most geographically-widespread species, Emergomyces africanus is endemic to Southern Africa and causes disseminated disease with cutaneous involvement primarily among patients with advanced human immunodeficiency virus (HIV) disease. Summary Emergomycosis, a disseminated clinical disease resulting from infection with dimorphic fungi in the genus Emergomyces, occurs primarily among immunocompromised patients. Further knowledge is needed on the pathophysiology, diagnosis and management of emergomycosis.
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  • 文章类型: Journal Article
    Recently, the global emergence of emergomycosis, a systemic fungal infection caused by a novel dimorphic fungus Emergomyces species has been observed among immunocompromised individuals. Though initially classified under the genus Emmonsia, a taxonomic revision in 2017 based on DNA sequence analyses placed five Emmonsia-like fungi under a separate genus Emergomyces. These include Emergomyces pasteurianus, Emergomyces africanus, Emergomyces canadensis, Emergomyces orientalis, and Emergomyces europaeus. Emmonsia parva was renamed as Blastomyces parvus, while Emmonsia crescens and Emmonsia sola remained within the genus Emmonsia until a taxonomic revision in 2020 placed both the species under the genus Emergomyces. However, unlike other members of the genus, Emergomyces crescens and Emergomyces sola do not cause disseminated disease. The former causes adiaspiromycosis, a granulomatous pulmonary disease, while the latter has not been associated with human disease. So far, emergomycosis has been mapped across four continents: Asia, Europe, Africa and North America. However, considering the increasing prevalence of HIV/AIDS, it is presumed that the disease must have a worldwide distribution with many cases going undetected. Diagnosis of emergomycosis remains challenging. It should be considered in the differential diagnosis of histoplasmosis as there is considerable clinical and histopathological overlap between the two entities. Sequencing the internal transcribed spacer region of ribosomal DNA is considered as the gold standard for identification, but its application is compromised in resource limited settings. Serological tests are non-specific and demonstrate cross-reactivity with Histoplasma galactomannan antigen. Therefore, an affordable, accessible, and reliable diagnostic test is the need of the hour to enable its diagnosis in endemic regions and also for epidemiological surveillance. Currently, there are no consensus guidelines for the treatment of emergomycosis. The recommended regimen consists of amphotericin B (deoxycholate or liposomal formulation) for 1-2 weeks, followed by oral itraconazole for at least 12 months. This review elaborates the taxonomic, clinical, diagnostic, and therapeutic aspects of emergomycosis. It also enumerates several novel antifungal drugs which might hold promise in the treatment of this condition and therefore, can be potential areas of future studies.
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  • 文章类型: Evaluation Study
    尿液中的组织胞浆抗原检测是播散性组织胞浆菌病的快速诊断方法,尽管在其他热双态真菌感染患者的标本中已经报道了交叉反应性。我们测试了尿液样本,怀疑有侵袭性真菌感染的人,2014年8月至2018年12月在南非国家真菌学参考实验室使用商业单克隆抗体组织血浆酶免疫测定法(EIA).从电子实验室信息系统获得相应的真菌培养和组织病理学结果。在某些情况下,培养的真菌分离株与尿液标本一起发送,以通过表型和分子方法进行物种水平鉴定。使用几种真菌病原体的培养滤液确认交叉反应性。在212个移交案件中,41(19%)被排除,因为他们没有记录的临床病史(n=1),替代诊断得到证实(n=2),或无真菌培养或组织病理学结果(n=38)。212人中有87人(41%)有侵袭性真菌病的实验室证据,而84(40%)没有。在87个案例中,37(43%)是培养证实的真菌病:初生菌病(n=18),组织胞浆菌病(n=8),孢子丝菌病(n=6),隐球菌病(n=2),真菌病(n=1),和其他真菌分离(n=2)。计算了两组的EIA的敏感性和特异性:培养证实(n=37)和组织学证实的侵袭性真菌病(n=50)。与培养物相比,EIA诊断组织胞浆菌病的敏感性和特异性分别为88%(7/8,95CI47-100%)和72%(21/29,95CI53-87%),分别,与组织学相比,诊断为急性真菌病/组织胞浆菌病的比例为83%(29/35,95CI66-93%)和93%(14/15,95CI68-100%),分别。发生交叉反应的患者的尿液标本与非洲产卵菌的培养滤液,马内菲T.和Blastomyces物种。商业组织胞浆EIA对培养证实的组织胞浆菌病的诊断具有令人满意的准确性,但是在由密切相关的病原体引起的侵袭性疾病患者的尿液标本中发生交叉反应,非洲E.Africanus和其他相关真菌的培养滤液。
    在CD4细胞计数低的HIV-血清反应阳性的人中,非洲胚和荚膜组织胞浆是引起多系统疾病的真菌。处理这些真菌的活培养物以确认诊断需要专门的实验室设备和基础设施,这在低资源环境中很少使用。这两种疾病的特征(即,播散性组织胞浆菌病和胚真菌病)在制备受感染的组织时可能无法区分,染色,并在显微镜下检查。酶免疫测定(EIA)已被开发为快速诊断工具,用于检测尿液标本中荚膜H.尽管在其他真菌感染患者的标本中已经报道了交叉反应。我们评估了商业组织胞浆菌EIA诊断组织胞浆菌病的准确性,并评估了来自胚乳菌病患者的尿液标本以及非洲E.Africanus和相关真菌培养物中的交叉反应。我们报告了与培养物相比,组织胞浆菌病诊断的敏感性和特异性分别为88%(95CI47-100%)和72%(95CI53-87%),而与通过显微镜检查感染组织的诊断相比,用于诊断组织胞浆病/母菌病的敏感性和特异性分别为83%(95CI66-93%)和93%(95CI68-100%)。该测定法在来自白菌病患者的尿液标本和相关真菌的培养滤液中发生交叉反应。尽管EIA与其他相关真菌发生交叉反应,该试验可缩短诊断时间,并有助于南非的胚芽菌病和组织胞浆菌病的早期治疗.
    Histoplasma antigen detection in urine is a rapid diagnostic method for disseminated histoplasmosis, although cross-reactivity has been reported in specimens from patients with other thermally dimorphic fungal infections. We tested urine specimens, from persons with suspected invasive fungal infections, using a commercial monoclonal antibody Histoplasma enzyme immunoassay (EIA) at a South African national mycology reference laboratory from August 2014 through December 2018. Corresponding fungal culture and histopathology results were obtained from an electronic laboratory information system. In some cases, cultured fungal isolates were sent with the urine specimen for species-level identification by phenotypic and molecular methods. Cross-reactivity was confirmed using culture filtrates of several fungal pathogens. Of 212 referred cases, 41 (19%) were excluded since they had no recorded clinical history (n = 1), alternative diagnoses were confirmed (n = 2), or no fungal culture or histopathology results (n = 38). Eighty-seven of 212 (41%) had laboratory evidence of an invasive fungal disease, while 84 (40%) did not. Of the 87 cases, 37 (43%) were culture-confirmed mycoses: emergomycosis (n = 18), histoplasmosis (n = 8), sporotrichosis (n = 6), cryptococcosis (n = 2), talaromycosis (n = 1), and other fungi isolated (n = 2). The sensitivity and specificity of the EIA were calculated for two groups: culture-confirmed (n = 37) and histology-confirmed invasive fungal disease (n = 50). The sensitivity and specificity of the EIA for diagnosis of histoplasmosis compared to culture were 88% (7/8, 95%CI 47-100%) and 72% (21/29, 95%CI 53-87%), respectively, and for diagnosis of emergomycosis/histoplasmosis compared to histology was 83% (29/35, 95%CI 66-93%) and 93% (14/15, 95%CI 68-100%), respectively. Cross-reactions occurred in urine specimens of patients with Emergomyces africanus infection and in culture filtrates of E. africanus, T. marneffei and Blastomyces species. A commercial Histoplasma EIA had satisfactory accuracy for diagnosis of culture-confirmed histoplasmosis, but cross-reacted in urine specimens from patients with invasive disease caused by the closely-related pathogen, E. africanus and in culture filtrates of E. africanus and other related fungi.
    UNASSIGNED: Emergomyces africanus and Histoplasma capsulatum are fungi that cause a multi-system disease among HIV-seropositive persons with a low CD4 cell count. Handling live cultures of these fungi to confirm a diagnosis requires specialized laboratory equipment and infrastructure which is infrequently accessible in low-resource settings. The features of the two diseases (i.e., disseminated histoplasmosis and emergomycosis) may be indistinguishable when infected tissue is prepared, stained, and examined under a microscope. Enzyme immunoassays (EIA) have been developed as rapid diagnostic tools for the detection of a cell wall component of H. capsulatum in urine specimens, although cross-reactions have been reported in specimens from patients with other fungal infections. We evaluated the accuracy of a commercial Histoplasma EIA to diagnose histoplasmosis and to assess cross-reactions in urine specimens from persons with emergomycosis and in cultures of E. africanus and related fungi. We report a sensitivity and specificity of 88% (95%CI 47-100%) and 72% (95%CI 53-87%) for diagnosis of histoplasmosis compared to culture and 83% (95%CI 66-93%) and 93% (95%CI 68-100%) for diagnosis of either histoplasmosis/emergomycosis compared to a diagnosis made by microscopic examination of infected tissue. The assay cross-reacted in urine specimens from patients with emergomycosis and in culture filtrates of related fungi. Although the EIA cross-reacted with other related fungi, this test can decrease the time to diagnosis and facilitate early treatment of emergomycosis and histoplasmosis in South Africa.
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