Abstract
BackgroundTrypanosoma cruzi, causative agent of Chagas disease, displays high intraspecific genetic diversity: six genetic lineages or discrete typing units (DTUs) are currently recognized, termed TcI through TcVI. Each DTU presents a particular distribution pattern across the Americas, and is loosely associated with different transmission cycles and hosts. Several DTUs are known to circulate in Central America. It has been previously suggested that TcI infection is benign and does not lead to chronic chagasic cardiomyopathy (CCC).FindingsIn this study, we genotyped T. cruzi parasites circulating in the blood and from explanted cardiac tissue of an El Salvadorian patient who developed reactivation Chagas disease while on immunosuppressive medications after undergoing heart transplant in the U.S. as treatment for end-stage CCC. Parasite typing was performed through molecular methods (restriction fragment length polymorphism of polymerase reaction chain amplified products, microsatellite typing, maxicircle sequence typing and low-stringency single primer PCR, [LSSP-PCR]) as well as lineage-specific serology. We show that the parasites infecting the patient belong to the TcI DTU exclusively. Our data indicate that the parasites isolated from the patient belong to a genotype frequently associated with human infection throughout the Americas (TcIDOM).ConclusionsOur results constitute compelling evidence in support of TcI DTU’s ability to cause end-stage CCC and help dispel any residual bias that infection with this lineage is benign, pointing to the need for increased surveillance for dissemination of this genotype in endemic regions, the USA and globally.
Highlights
Trypanosoma cruzi, causative agent of Chagas disease, displays high intraspecific genetic diversity: six genetic lineages or discrete typing units (DTUs) are currently recognized, termed Trypanosoma cruzi lineage I (TcI) through TcVI
Chagas disease, caused by Trypanosoma cruzi, is the most important parasitic disease in Latin America, [1] and constitutes an emerging global public health problem, since thousands of T. cruzi- infected Latin Americans migrated during the last few decades and live in North America, Europe, Australia, Japan and other regions [2]
There are as yet no proven associations between T. cruzi genetic lineages and the clinical presentations of the disease; DTUs TcII, V and VI are frequently reported to be present in the Southern Cone of South America where serious chronic manifestations include megaesophagus and megacolon, whereas TcI is reported to predominate in endemic countries north of the Amazon [4]
Summary
Trypanosoma cruzi, causative agent of Chagas disease, displays high intraspecific genetic diversity: six genetic lineages or discrete typing units (DTUs) are currently recognized, termed TcI through TcVI. * Correspondence: jacostalesc@puce.edu.ec 1Centro de Investigación en Enfermedades Infecciosas, Escuela de Biología, Pontificia Universidad Católica del Ecuador, Avenida 12 de Octubre y Roca, Quito, Ecuador Full list of author information is available at the end of the article to influence the clinical outcome.
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