Ten-year follow-up of the largest oral Chagas disease outbreak. Laboratory biomarkers of infection as indicators of therapeutic failure

Zoraida Díaz-Bello; Belkisyolé Alarcón de Noya; Arturo Muñoz-Calderón; Raiza Ruiz-Guevara; Luciano Mauriello; Cecilia Colmenares; Eyleen Moronta; Milagros Aponte; José Luis Ramírez; Oscar Noya-González

doi:10.1016/j.actatropica.2021.106034

Ten-year follow-up of the largest oral Chagas disease outbreak. Laboratory biomarkers of infection as indicators of therapeutic failure

Acta Trop. 2021 Oct:222:106034. doi: 10.1016/j.actatropica.2021.106034. Epub 2021 Jul 2.

Affiliations

¹ Instituto de Medicina Tropical, Facultad de Medicina, Universidad Central de Venezuela, Venezuela. Electronic address: zoraida_diaz@yahoo.com.
² Instituto de Medicina Tropical, Facultad de Medicina, Universidad Central de Venezuela, Venezuela.
³ Cátedra de Parasitología, Escuela de Medicina "Luis Razetti", Venezuela.
⁴ Centro de Biotecnología, Fundación Instituto de Estudios Avanzados, Venezuela.
⁵ Instituto de Medicina Tropical, Facultad de Medicina, Universidad Central de Venezuela, Venezuela; Centro de Estudios sobre Malaria, Instituto de Altos Estudios, Ministerio del Poder Popular para la Salud, Venezuela.

PMID: 34224715
DOI: 10.1016/j.actatropica.2021.106034

Abstract

Trypanosoma cruzi uses various mechanisms of infection to access humans. Since 1967, food contaminated with metacyclic trypomastigotes has triggered several outbreaks of acute infection of Chagas disease by oral transmission. Follow-up studies to assess the effectiveness of anti-parasitic treatment of oral outbreaks are rather scarce. Here, we report a 10-year laboratory follow-up using parasitological, serological, and molecular tests of 106 individuals infected in 2007 of the largest known outbreak of orally transmitted Chagas disease, which occurred in Caracas city, Venezuela. Before treatment (2007), specific IgA, IgM and IgG, were found in 71% (75/106), 90% (95/106) and 100% (106/106), respectively, in addition to 21% (9/43) parasitemia, Complement Mediated Lysis (CML) in 98% (104/106) and 79% (34/43) parasitic DNA for PCR. Blood culture detected parasitemia up to 18 months post-treatment in 6% (6/106) of the patients. In 2017, the original number of cases in the follow-up decreased by 46% and due to the country's economic situation, not all the trials could be carried out in the entire population. During follow-up, IgA and IgM disappeared promptly, with IgM persisting in 19% (20/104) of the patients three years after treatment. The anti-T. cruzi IgG remained positive 10 years later in 41% (20/49) of the individuals evaluated. CML remained positive seven years later in 79% (65/82) of the cases. PCR positive cases decreased after treatment but progressively recovered, being positive in 69% (32/46) of the individuals evaluated in 2017. The group of children (under 18 years of age) showed the highest PCR positivity with 76% (26/34) of the cases, but their parasitic load tended to diminish, while in adults the parasitic load regained their initial values. The simultaneous evaluation of serological tests and PCR of the patients allowed us to separate patients among responders and non-responders to the anti-parasitic treatment, and this information prompted us to apply a second anti-parasitic treatment in the group of non-responders. In this population not subjected to the like lihood of re-infection, adult patients were more likely to be non-responders when compared to children. These results suggest that rigorous laboratory follow-up with T. cruzi infectious biomarkers is essential to detect cases of parasite persistence.

Keywords: Anti-parasitic treatment; Follow-up; Humoral immune response; Oral Chagas disease; Therapeutic failure; Venezuela.

MeSH terms

Adult
Antibodies, Protozoan / analysis
Biomarkers
Chagas Disease* / diagnosis
Chagas Disease* / drug therapy
Chagas Disease* / epidemiology
Child
Disease Outbreaks
Follow-Up Studies
Humans
Seroepidemiologic Studies
Treatment Failure
Venezuela / epidemiology

Substances

Antibodies, Protozoan
Biomarkers