Genetic polymorphism of Trypanosoma cruzi bloodstream populations in adult chronic indeterminate Chagas disease patients from the E1224 clinical trial

Author:

Ramírez Juan Carlos1,Acevedo Gonzalo Raúl1,Torres Carolina23,Parrado Rudy4,De La Barra Anabelle4,Villarroel Sandro4,García Lineth4,Gascon Joaquim5,Ortiz Lourdes6,Torrico Faustino7,Ribeiro Isabela8,Schijman Alejandro Gabriel1

Affiliation:

1. Instituto de Investigaciones en Ingeniería Genética y Biología Molecular “Dr. Héctor N. Torres” (INGEBI-CONICET), Buenos Aires, Argentina

2. Universidad de Buenos Aires, Instituto de Investigaciones en Bacteriología y Virología Molecular (IBaViM), Buenos Aires, Argentina

3. Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina

4. Instituto de Investigaciones Biomédicas (IIBISMED), Universidad Mayor de San Simón, Cochabamba, Bolivia

5. ISGlobal, Barcelona Centre for International Health Research (CRESIB), Hospital Clínic-Universitat de Barcelona, Barcelona, Spain

6. Universidad Autónoma Juan Misael Saracho, Tarija, Bolivia

7. Colectivo de Estudios Aplicados y Desarrollo Social (CEADES), Cochabamba, Bolivia

8. Drugs for Neglected Diseases initiative (DNDi), Geneva, Switzerland

Abstract

Abstract Background The role that the genetic diversity of natural Trypanosoma cruzi populations plays in response to trypanocidal treatment of chronic Chagas disease (CD) patients remains to be understood. We analysed the genetic polymorphisms of parasite bloodstream populations infecting chronic CD patients enrolled in the E1224 clinical trial. Methods A total of 506 baseline and post-treatment follow-up samples from 188 patients were analysed. T. cruzi satellite DNA (satDNA) was amplified and sequenced using cruzi1/cruzi2 primers, and samples with TcI/III, TcII, TcIV or hybrid satDNA sequences were identified. Minicircle signatures were obtained after kinetoplast DNA amplification using 121/122 primers and restriction enzyme digestion. Genetic distances between baseline and post-treatment minicircle signatures were estimated using the Jaccard coefficient. Results At baseline, 74.3% TcII, 17.9% hybrid and 7.8% TcI/III satDNA sequences were found, whereas at the end of follow-up the distribution was 55.2% TcII, 35.2% hybrid and 9.5% TcI/III. The placebo arm was the treatment group with the highest variation of satDNA sequences between baseline and post-treatment follow-up. Genetic distances between baseline and post-treatment minicircle signatures were similar among all treatment arms. No association between minicircle signature variability and satDNA type distribution was found. Conclusions Genetic variability of T. cruzi bloodstream populations during post-treatment follow-up did not differ from that observed during chronic infection in the absence of treatment, suggesting that there were no selection events of E1224-resistant parasite populations. This is the first report documenting the genetic polymorphism of natural T. cruzi populations in chronic patients in the context of clinical trials with trypanocidal drugs.

Funder

National Agency of Science, Technology and Productive Innovation

Wellcome Trust

Médecins Sans Frontières, International

Ministry of Foreign Affairs, Spain

Department for International Development (DFID), UK

Dutch Ministry of Foreign Affairs (DGIS), Netherlands

Rockefeller Foundation, USA

Federal Ministry of Education and Research (BMBF) through KfW, Germany

CEADES Foundation, Bolivia

Universidad Mayor de San Simon, Bolivia

Universidad Juan Misael Saracho, Bolivia

ISGlobal (Barcelona Institute for Global Health), Spain

Spanish Agency for Cooperation and Development

Agència de Gestió d’Ajuts Universitaris i de Recerca

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology,Microbiology (medical)

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