Dhanalakshmi Solaimalai, Rosemol Varghese, Sujith Karumathil, Uday Kulkarni, Biju George, Joy Sarojini Michael
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The patients were categorised into probable, possible, and no IA based on revised (2020) and previous (2008) European Organization for Research and Treatment of Cancer and the National Institute of Allergy and Infectious Diseases Mycoses Study Group (EORTC-MSG) criteria. The performance characteristics of PCR and GM were calculated against the EORTC criteria by combining probable and possible cases as diseased groups. Among the 107 recruited patients, 93 were categorised into probable/possible IA (diseased group) and 14 into no IA group. The PCR was positive in 53 samples from 49 patients. The sensitivity and specificity of single positive PCR and GM were 51.61% [95% confidence interval, 41-62], 92.86% (66.1-99.8) and 26.88% (18.2-37.1), 92.86% (66.1-99.8), respectively. The combination-based strategy (GM and/or PCR positive) exhibited a moderate sensitivity of 62.37% (51-72.2) and a specificity of 85.71% (57.2-98.2). 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引用次数: 0
摘要
侵袭性曲霉菌病(IA)是血液肿瘤科高危患者的一种潜在致命感染。由于传统诊断方法存在许多固有难题,聚合酶链反应(PCR)一直被用于诊断侵袭性曲霉菌病。这项前瞻性研究评估了商用 AsperGenius 多路实时 PCR 与半乳甘露聚糖检测临床疑似 IA 的血液肿瘤患者血清样本的临床实用性。2022 年 4 月至 2023 年 3 月期间,共招募了 107 名患者。通过半乳甘露聚糖酶联免疫吸附试验(ELISA)进行常规诊断的患者的血清样本(n=113)进行了 PCR 检测。根据修订版(2020 年)和之前(2008 年)的 EORTC-MSG 标准,将患者分为可能、可能和无 IA 三类。根据 EORTC 标准计算了 PCR 和半乳甘露聚糖的性能特征,将可能和可能的病例合并为患病组。在招募的 107 名患者中,93 人被归入可能/可能的内脏癌(患病组),14 人被归入无内脏癌组。在 49 名患者的 53 份样本中,PCR 检测结果呈阳性。单一阳性 PCR 和半乳甘露聚糖的敏感性和特异性分别为 51.61% (95% CI, 41 to 62), 92.86% (66.1 to 9.8) 和 26.88% (18.2 to 37.1), 92.86% (66.1 to 99.8)。基于联合策略(GM 和/或 PCR 阳性)的灵敏度为 62.37%(51-72.2),特异性为 85.71%(57.2-98.2)。总之,血清 GM 和/或 PCR 阳性与符合 EORTC/MSG 标准的放射学检查结果相结合的策略提高了临床疑似 IA 的高危血液病患者对可能 IA 的诊断率。
Diagnosis of invasive aspergillosis in haemato-oncology patients in a routine diagnostic setting.
Invasive Aspergillosis (IA) is a potentially lethal infection in high-risk haemato-oncology patients. Since traditional diagnostic methods have many inherent challenges, Polymerase Chain Reaction (PCR) has been used to diagnose IA. This prospective study evaluated a commercial AsperGenius multiplex real-time PCR for its clinical utility in diagnosing IA compared with galactomannan (GM) testing serum samples from haemato-oncology patients with clinically suspected IA. A total of 107 patients were recruited between April 2022 and March 2023. Serum samples (n = 113) collected from those patients for the routine diagnosis by GM Enzyme Linked Immuno-Sorbent Assay (ELISA) were subjected to PCR. The patients were categorised into probable, possible, and no IA based on revised (2020) and previous (2008) European Organization for Research and Treatment of Cancer and the National Institute of Allergy and Infectious Diseases Mycoses Study Group (EORTC-MSG) criteria. The performance characteristics of PCR and GM were calculated against the EORTC criteria by combining probable and possible cases as diseased groups. Among the 107 recruited patients, 93 were categorised into probable/possible IA (diseased group) and 14 into no IA group. The PCR was positive in 53 samples from 49 patients. The sensitivity and specificity of single positive PCR and GM were 51.61% [95% confidence interval, 41-62], 92.86% (66.1-99.8) and 26.88% (18.2-37.1), 92.86% (66.1-99.8), respectively. The combination-based strategy (GM and/or PCR positive) exhibited a moderate sensitivity of 62.37% (51-72.2) and a specificity of 85.71% (57.2-98.2). To conclude, the combined strategy of serum GM and/or PCR positivity, along with radiological findings that fulfilled the EORTC/MSG criteria, has improved the diagnosis of probable IA among high-risk haematological patients with clinically suspected IA.
期刊介绍:
Medical Mycology is a peer-reviewed international journal that focuses on original and innovative basic and applied studies, as well as learned reviews on all aspects of medical, veterinary and environmental mycology as related to disease. The objective is to present the highest quality scientific reports from throughout the world on divergent topics. These topics include the phylogeny of fungal pathogens, epidemiology and public health mycology themes, new approaches in the diagnosis and treatment of mycoses including clinical trials and guidelines, pharmacology and antifungal susceptibilities, changes in taxonomy, description of new or unusual fungi associated with human or animal disease, immunology of fungal infections, vaccinology for prevention of fungal infections, pathogenesis and virulence, and the molecular biology of pathogenic fungi in vitro and in vivo, including genomics, transcriptomics, metabolomics, and proteomics. Case reports are no longer accepted. In addition, studies of natural products showing inhibitory activity against pathogenic fungi are not accepted without chemical characterization and identification of the compounds responsible for the inhibitory activity.