The molecular repertoire of effects its virulence and impacts the clinical course of the resulting Chagas disease. This study aimed to determine the mechanism underlying the pathogenicity of . Two cell lines (C8C3 and C8C3), obtained from the clone H510 C8C3 and exhibiting different virulence phenotypes, were used to evaluate the parasite's infectivity in mice. The organ parasite load was analysed by qPCR. The proteomes of both cell lines were compared using nLC-MS/MS. Cruzipain (Czp), complement regulatory protein (CRP), trans-sialidase (TS), Tc-85, and sialylated epitope expression levels were evaluated by immunoblotting. High-virulence C8C3 was highly infectious in mice and demonstrated three to five times higher infectivity in mouse myocardial cells than low-virulence C8C3. qPCR revealed higher parasite loads in organs of acute as well as chronically C8C3-infected mice than in those of C8C3-infected mice. Comparative quantitative proteomics revealed that 390 of 1547 identified proteins were differentially regulated in C8C3 with respect to C8C3. Amongst these, 174 proteins were upregulated in C8C3 and 216 were downregulated in C8C3. The upregulated proteins in C8C3 were associated with the tricarboxylic acid cycle, ribosomal proteins, and redoxins. Higher levels of Czp, CRP, TS, Tc-85, and sialylated epitopes were expressed in C8C3 than in C8C3. Thus, virulence may be related to virulence factor expression as well as upregulation of bioenergetic and biosynthetic pathways proteins.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9601562PMC
http://dx.doi.org/10.1080/21505594.2022.2132776DOI Listing

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