Serological reactivity against T. cruzi-derived antigens: Evaluation of their suitability for the assessment of response to treatment in chronic Chagas disease

•Early markers of therapeutic efficacy are essential for Chagas disease control.•A blinded case-control study for analysis of T. cruzi antigens is described.•Sera from a retrospective cohort of T. cruzi-infected and controls were used.•KMP11, 3973 and PFR2 obeyed the recent TPP criteria for Se (≥60%...

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Published in:Acta tropica 2021-09, Vol.221, p.105990-105990, Article 105990
Main Authors: Alonso-Padilla, Julio, López, Manuel Carlos, Esteva, Mónica, Zrein, Maan, Casellas, Aina, Gómez, Inmaculada, Granjon, Elodie, Méndez, Susana, Benítez, Celia, Ruiz, Andres Mariano, Sanz, Sergi, Gascón, Joaquim, Thomas, M Carmen, Pinazo, Maria-Jesus, Abril, Marcelo, de Noya, Belkisyolé Alarcón, Jorge, Tania Araujo, Chatelain, Eric, Grijalva, Mario J., Guhl, Felipe, Hasslocher-Moreno, Alejandro Marcel, Luquetti, Alejandro O., Noya, Oscar, Ramsey, Janine M., Ribeiro, Isabela, Longhi, Silvia A., Schijman, Alejandro G., Sosa-Estani, Sergio, Torrico, Faustino, Viotti, Rodolfo
Format: Article
Language:English
Subjects:
3973
Antigens
Chagas disease
Chemotherapy response
Chronic infection
F29
HSP70
InfYnity multiplexed ELISA
KMP11
PFR2
Trypanosoma cruzi
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Summary:•Early markers of therapeutic efficacy are essential for Chagas disease control.•A blinded case-control study for analysis of T. cruzi antigens is described.•Sera from a retrospective cohort of T. cruzi-infected and controls were used.•KMP11, 3973 and PFR2 obeyed the recent TPP criteria for Se (≥60%) and Sp (≥90%).•T. cruzi KMP11 and 3973 antigens showed a good post-treatment reactivity decline. Chagas disease, caused by the protozoan Trypanosoma cruzi, affects more than 6 million people worldwide. Following a mostly asymptomatic acute phase, the disease progresses to a long-lasting chronic phase throughout which life-threatening disorders to the heart and/or gastrointestinal tract will manifest in about 30% of those chronically infected. During the chronic phase, the parasitemia is low and intermittent, while a high level of anti-T. cruzi antibodies persist for years. These two features hamper post-chemotherapeutic follow-up of patients with the tools available. The lack of biomarkers for timely assessment of therapeutic response discourages a greater use of the two available anti-parasitic drugs, and complicates the evaluation of new drugs in clinical trials. Herein, we investigated in a blinded case-control study the serological reactivity over time of a group of parasite-derived antigens to potentially address follow up of T. cruzi chronically infected subjects after treatment. We tested PFR2, KMP11, HSP70, 3973, F29 and the InfYnity multiplexed antigenic array, by means of serological assays on a multi-national retrospective collection of samples. Some of the antigens exhibited promising results, underscoring the need for further studies to determine their potential role as treatment response biomarkers.
ISSN:0001-706X
1873-6254
DOI:10.1016/j.actatropica.2021.105990