M. Pinazo, Colin J. Forsyth, Constanza Lopez-Albizu, M. Bisio, Adriana González-Martínez, Laura Bohorquez, Jimy Pinto, Israel Molina, A. Marchiol, Rafael Herazo, I. Galván, Tayná Marques, Fabiana Barreira, Juan Carlos Villar, Yanina Sguassero, Maria Soledad Santini, J. Altcheh, B. Alarcón de Noya, S. Sosa-Estani
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In newborns at risk of vertical transmission, simplified diagnostic algorithms that provide timely results can reduce the high follow-up losses observed with current algorithms. Molecular methods have also proved useful for monitoring T. cruzi infection in solid organ transplantation recipients, regardless of host immune status, allowing parasite detection even before symptom manifestation. Furthermore, in the absence of other biomarkers and a practical test of cure, and given the limitations of serological methods, recent clinical guidelines have included polymerase chain reaction (PCR) to detect therapeutic failure after antiparasitic treatment in chronically infected adults. Increasing evidence supports the use of molecular tests in a clinical context, given the improved sensitivity and specificity of current assays – characteristics which largely depend on epidemiological factors and genetic and antigenic variability among T. cruzi strains. 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引用次数: 0
摘要
克鲁兹锥虫感染可通过寄生虫学、分子和血清学检测进行诊断。以 DNA 扩增为基础的分子方法比传统的寄生虫学技术更灵敏,可用于检测克鲁兹锥虫寄生虫血症的证据,是先天性和经口传播病例以及慢性感染的免疫抑制患者寄生虫再活化的首选检测方法。对于有垂直传播风险的新生儿,能及时提供结果的简化诊断算法可减少目前算法中观察到的高随访损失。事实证明,分子方法对于监测实体器官移植受者的 T. cruzi 感染也很有用,无论宿主的免疫状态如何,甚至在症状出现之前就能检测到寄生虫。此外,由于缺乏其他生物标志物和实用的治愈检测方法,并考虑到血清学方法的局限性,近期的临床指南已将聚合酶链反应(PCR)纳入其中,用于检测慢性感染成人抗寄生虫治疗后的治疗失败情况。鉴于目前检测方法的灵敏度和特异性有所提高,越来越多的证据支持在临床中使用分子检测方法,而这些特点在很大程度上取决于流行病学因素以及 T. cruzi 菌株之间的遗传和抗原变异性。商业 PCR 试剂盒的进一步开发和注册将提高分子检测的使用率。我们讨论了 PCR 和其他分子检验在临床管理中对 T. cruzi 感染者的作用。
Clinical use of molecular methods for Trypanosoma cruzi infection in endemic and non-endemic countries: Benefits, limitations and challenges
Trypanosoma cruzi infection is diagnosed by parasitological, molecular, and serological tests. Molecular methods based on DNA amplification provide a more sensitive alternative to classical parasitological techniques for detecting evidence of T. cruzi parasitemia, and are the preferred tests for congenital and oral transmission cases and parasite reactivation in chronically infected immunosuppressed individuals. In newborns at risk of vertical transmission, simplified diagnostic algorithms that provide timely results can reduce the high follow-up losses observed with current algorithms. Molecular methods have also proved useful for monitoring T. cruzi infection in solid organ transplantation recipients, regardless of host immune status, allowing parasite detection even before symptom manifestation. Furthermore, in the absence of other biomarkers and a practical test of cure, and given the limitations of serological methods, recent clinical guidelines have included polymerase chain reaction (PCR) to detect therapeutic failure after antiparasitic treatment in chronically infected adults. Increasing evidence supports the use of molecular tests in a clinical context, given the improved sensitivity and specificity of current assays – characteristics which largely depend on epidemiological factors and genetic and antigenic variability among T. cruzi strains. Further development and registration of commercial PCR kits will improve the use of molecular tests. We discuss the attributes of PCR and other molecular tests for clinical management in people with T. cruzi infection.