Abstract
.The existence of an imperfect reference standard presents complications when evaluating the unbiased performance of novel diagnostic techniques. This is especially true in the absence of a gold standard, as is the case in chronic Chagas disease (CD) diagnosis. To circumvent this constraint, we elected to use latent class analysis (LCA). Previously, our group demonstrated the high performance of four Trypanosoma cruzi–chimeric proteins (Molecular Biology Institute of Paraná [IBMP]-8.1, -8.2, -8.3, and -8.4) for CD diagnosis using several distinct immunoassays. Although commercial tests had previously been established as a reference standard, the diagnostic performance of these chimeric antigens could present bias because these tests fail to produce 100% accurate results. Thus, we used LCA to assess the performance of these IBMP chimeric antigens in chronic CD diagnosis. Using the LCA model as a gold standard, sensitivity and specificity values ranged from 93.5% to 99.4% and 99.6% to 100%, respectively. The accuracy values were 96.2% for IBMP-8.2, approximately 98% for IBMP-8.1 and IBMP-8.3, and nearly 100% for IBMP-8.4. For IBMP-8.1 and IBMP-8.2, higher positive predictive values were associated with increases in hypothetical prevalence. Similarly, higher hypothetical prevalence resulted in lower negative predictive values for IBMP-8.1, IBMP-8.2, and IBMP-8.3. In addition, samples with serodiscordant results from commercial serological tests were analyzed using LCA. Molecular Biology Institute of Paraná -8.1 demonstrated potential for use in confirmatory testing with regard to samples with inconsistent results. Moreover, our findings further confirmed the remarkable performance of the IBMP-8.4 antigen to diagnose chronic CD in both endemic and non-endemic areas.
Highlights
Chagas disease (CD), a life-threatening condition arising from the hemoflagellated protozoan Trypanosoma cruzi, represents a major health problem in Latin America.[1]
Samples were considered as Ch-positive when at least two chimeric antigens presented positivity (P3–P5), with posteriori probability (PP) > 87%
A latent class model was used to estimate the diagnostic performance of four recombinant chimeric antigenic proteins to precisely detect anti–T. cruzi antibodies
Summary
Chagas disease (CD), a life-threatening condition arising from the hemoflagellated protozoan Trypanosoma cruzi, represents a major health problem in Latin America.[1]. Considering the fact that CD is characterized by a prolonged asymptomatic phase and that most affected individuals reside in peri-urban slums or rural areas, improvements in measures to control and prevent CD must be made. Because most chagasic (Ch) individuals in the ongoing chronic phase are never tested and remain unaware of their condition, it is essential to develop accurate CD diagnostic tools for use both in routine health services and at blood centers. Direct microscopic observation of trypomastigote forms is the preferred method to affirm diagnosis as a result of high parasite load in the blood. In this phase, indirect serological methodologies present low sensitivity due to a delayed humoral immune response.[10] Symptoms present
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