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Incomplete Recruitment of Protective T Cells Is Associated with Trypanosoma cruzi Persistence in the Mouse Colon

Alexander I. Ward, Michael D. Lewis, Martin C. Taylor, John M. Kelly

2021Infection and Immunity15 citationsDOIOpen Access PDF

Abstract

Trypanosoma cruzi is the etiological agent of Chagas disease. Following T cell-mediated suppression of acute-phase infection, this intracellular eukaryotic pathogen persists long-term in a limited subset of tissues at extremely low levels. The reasons for this tissue-specific chronicity are not understood. Using a dual bioluminescent-fluorescent reporter strain and highly sensitive tissue imaging that allows experimental infections to be monitored at single-cell resolution, we undertook a systematic analysis of the immunological microenvironments of rare parasitized cells in the mouse colon, a key site of persistence. We demonstrate that incomplete recruitment of T cells to a subset of colonic infection foci permits the occurrence of repeated cycles of intracellular parasite replication and differentiation to motile trypomastigotes at a frequency sufficient to perpetuate chronic infections. The lifelong persistence of parasites in this tissue site continues despite the presence, at a systemic level, of a highly effective T cell response. Overcoming this low-level dynamic host-parasite equilibrium represents a major challenge for vaccine development.

Topics & Concepts

BiologyTrypanosoma cruziIntracellularPathogenPersistence (discontinuity)VirologyIntracellular parasiteViral replicationKinetoplastidaImmunologyChagas diseaseImmune systemParasite hostingMicrobiologyImmunityStrain (injury)Cell cultureCellPhenotypeChronic infectionTrypanosomaEtiologyT cellTrypanosoma species research and implicationsT-cell and Retrovirus StudiesDiabetes and associated disorders
Incomplete Recruitment of Protective T Cells Is Associated with Trypanosoma cruzi Persistence in the Mouse Colon | Litcius