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首页> 外文期刊>Journal of Clinical Microbiology >Cross-Reactivity Using Chimeric Trypanosoma cruzi Antigens: Diagnostic Performance in Settings Where Chagas Disease and American Cutaneous or Visceral Leishmaniasis Are Coendemic
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Cross-Reactivity Using Chimeric Trypanosoma cruzi Antigens: Diagnostic Performance in Settings Where Chagas Disease and American Cutaneous or Visceral Leishmaniasis Are Coendemic

机译:使用嵌合克鲁斯锥虫抗原的交叉反应性:在南美锥虫病和美国皮肤或内脏利什曼病共同存在的环境中的诊断性能

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摘要

Chimeric T. cruzi antigens have been proposed as a diagnostic tool for chronic Chagas disease (CD) in both settings where Chagas disease is endemic and those where it is not endemic. Antibody response varies in accordance to each T. cruzi strain, presenting challenges to the use of antigens lacking demonstrated cross-reactivity with Leishmania spp. ABSTRACT Chimeric T. cruzi antigens have been proposed as a diagnostic tool for chronic Chagas disease (CD) in both settings where Chagas disease is endemic and those where it is not endemic. Antibody response varies in accordance to each T. cruzi strain, presenting challenges to the use of antigens lacking demonstrated cross-reactivity with Leishmania spp. Our group expressed four chimeric proteins (IBMP-8.1, IBMP-8.2, IBMP-8.3, and IBMP-8.4) and previously assessed their diagnostic performance to determine cross-reactivity with Leishmania spp. Here, we validated our findings using serum samples from different Brazilian geographic areas reporting endemic Chagas disease, endemic visceral or American cutaneous leishmaniasis (ACL), or both. Overall, 829 serum samples were evaluated using commercial and IBMP enzyme-linked immunosorbent assays. Due to the absence of a reference assay to diagnosis CD, latent class analysis (LCA) was performed through the use of a statistical model. The incidence of cross-reactivity for ACL-positive samples varied from 0.35% (IBMP-8.3) to 0.70% (IBMP-8.1 and IBMP-8.2). Regarding visceral leishmaniasis (VL)-positive samples, the IBMP-8.2 and IBMP-8.3 antigens cross-reacted with six (3.49%) and with only one sample (0.58%), respectively. No cross-reactivity with either ACL or VL was observed for the IBMP-8.4 antigen. Similarly, no cross-reactions were found when VL-positive samples were assayed with IBMP-8.1. The agreement among the results obtained using IBMP antigens ranged from 97.3% for IBMP-8.2 and 99% for IBMP-8.1 and IBMP-8.3 to 100% for IBMP-8.4, demonstrating almost perfect agreement with LCA. Accordingly, in light of the negligible cross-reactivity with both ACL and VL, we suggest the use of IBMP antigens in regions where T. cruzi and Leishmania spp. are coendemic.
机译:嵌合克鲁维氏锥虫抗原已被建议作为查加斯病的地方病和非特加斯病的慢性查加斯病(CD)的诊断工具。抗体反应随每个克鲁氏杆菌菌株的不同而不同,这给使用缺乏证明与利什曼原虫属物种具有交叉反应性的抗原提出了挑战。摘要在美洲锥虫病为地方病和非美洲锥虫病的两种情况下,已提出了嵌合克鲁氏锥虫抗原作为慢性南美锥虫病(CD)的诊断工具。抗体反应随每个克鲁氏杆菌菌株的不同而不同,这给使用缺乏证明与利什曼原虫属物种具有交叉反应性的抗原提出了挑战。我们的小组表达了四种嵌合蛋白(IBMP-8.1,IBMP-8.2,IBMP-8.3和IBMP-8.4),并事先评估了它们的诊断性能以确定与利什曼原虫的交叉反应性。在这里,我们使用来自巴西不同地区的血清样本证实了我们的发现,这些血清样本报告了地方性恰加斯病,地方性内脏或美国皮肤利什曼病(ACL),或两者都有。总体而言,使用商业和IBMP酶联免疫吸附测定法评估了829个血清样品。由于缺少诊断CD的参考检测,因此通过使用统计模型进行了潜在类别分析(LCA)。 ACL阳性样品的交叉反应发生率从0.35%(IBMP-8.3)到0.70%(IBMP-8.1和IBMP-8.2)不等。关于内脏利什曼病(VL)阳性样品,IBMP-8.2和IBMP-8.3抗原分别与六种(3.49%)和仅一种样品(0.58%)交叉反应。对于IBMP-8.4抗原,未观察到与ACL或VL的交叉反应。同样,当用IBMP-8.1分析VL阳性样品时,没有发现交叉反应。使用IBMP抗原获得的结果之间的一致性范围从IBMP-8.2的97.3%,IBMP-8.1和IBMP-8.3的99%到IBMP-8.4的100%不等,这表明与LCA的一致性非常好。因此,鉴于与ACL和VL的交叉反应可忽略不计,我们建议在克鲁氏梭菌和利什曼原虫属的地区使用IBMP抗原。是普遍的。

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