Abstract
Chronic Chagas cardiomyopathy (CCC) is the most frequent and severe form of Chagas disease, a neglected tropical illness caused by the protozoan Trypanosoma cruzi, and the main cause of morbimortality from cardiovascular problems in endemic areas. Although efforts have been made to understand the signaling pathways and molecular mechanisms underlying CCC, the immunological signaling pathways regulated by the etiological treatment with benznidazole (Bz) has not been reported. In experimental CCC, Bz combined with the hemorheological and immunoregulatory agent pentoxifylline (PTX) has beneficial effects on CCC. To explore the molecular mechanisms of Bz or Bz+PTX therapeutic strategies, C57BL/6 mice chronically infected with the T. cruzi Colombian strain (discrete typing unit TcI) and showing electrocardiographic abnormalities were submitted to suboptimal dose of Bz or Bz+PTX from 120 to 150 days postinfection. Electrocardiographic alterations, such as prolonged corrected QT interval and heart parasite load, were beneficially impacted by Bz and Bz+PTX. RT-qPCR TaqMan array was used to evaluate the expression of 92 genes related to the immune response in RNA extracted from heart tissues. In comparison with non-infected mice, 30 genes were upregulated, and 31 were downregulated in infected mice. Particularly, infection upregulated the cytokines IFN-γ, IL-12b, and IL-2 (126-, 44-, and 18-fold change, respectively) and the T-cell chemoattractants CCL3 and CCL5 (23- and 16-fold change, respectively). Bz therapy restored the expression of genes related to inflammatory response, cellular development, growth, and proliferation, and tissue development pathways, most probably linked to the cardiac remodeling processes inherent to CCC, thus mitigating the Th1-driven response found in vehicle-treated infected mice. The combined Bz+PTX therapy revealed pathways related to the modulation of cell death and survival, and organismal survival, supporting that this strategy may mitigate the progression of CCC. Altogether, our results contribute to the better understanding of the molecular mechanisms of the immune response in the heart tissue in chronic Chagas disease and reinforce that parasite persistence and dysregulated immune response underpin CCC severity. Therefore, Bz and Bz+PTX chemotherapies emerge as tools to interfere in these pathways aiming to improve CCC prognosis.
Highlights
Chagas disease (CD) or American trypanosomiasis is an infectious disease caused by the protozoan parasite Trypanosoma cruzi, responsible for an estimated 6 to 7 million people infected and approximately 75 million at risk of infection (World Health Organization, 2021)
Since molecular mechanisms in the immune response play an important part in CD, in the present study, using a welldescribed experimental model reproducing pivotal aspects of the cardiac form of CD in C57BL/6 mice infected with the T. cruzi Colombian (TcI) strain (Zingales, 2018), we investigate the immune molecular mechanisms involved in the CCC, using a RT-qPCR TaqMan array to evaluate the expression of 92 genes related to the immune response
To determine the effect of suboptimal dose of Bz and/or PTX on the molecular pattern of immune response in experimental CD heart disease, C57BL/6 mice were intraperitoneally infected with 100 blood-derived trypomastigotes (BDTs) (Colombian strain), which is a highly pathogenic parasite strain
Summary
Chagas disease (CD) or American trypanosomiasis is an infectious disease caused by the protozoan parasite Trypanosoma cruzi, responsible for an estimated 6 to 7 million people infected and approximately 75 million at risk of infection (World Health Organization, 2021). Chagas disease has a 4- to 8-week acute phase, characterized by patent parasitemia and inflammation due to tissue parasitism (Nunes et al, 2018), usually asymptomatic or causing broad symptoms manifestations as fever, enlargement of lymph nodes, and subcutaneous edema, which jeopardize a clear diagnosis (Rassi et al, 2012). Trypanocidal pharmacotherapy at this point is effective with a cure rate of 60% to 85% (Bern, 2011); the main problem, lies in diagnosing the disease and treating it at the right time. It is suggested that up to 5% of patients evolve each year to a clinical determinate form of CD, with 30% to 40% of the patients progressing to the chronic determinate forms of CD, with cardiac, digestive, or cardio-digestive manifestations (Sabino et al, 2013; Nunes et al, 2018)
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
