Murine colon organoids as a novel model to study Trypanosoma cruzi infection and interactions with the intestinal epithelium

Hellen Daghero; Romina Pagotto; Cristina Quiroga; Andrea Medeiros; Marcelo A Comini; Mariela Bollati-Fogolín

doi:10.3389/fcimb.2023.1082524

Murine colon organoids as a novel model to study Trypanosoma cruzi infection and interactions with the intestinal epithelium

Front Cell Infect Microbiol. 2023 Mar 9:13:1082524. doi: 10.3389/fcimb.2023.1082524. eCollection 2023.

Authors

Hellen Daghero¹, Romina Pagotto¹, Cristina Quiroga², Andrea Medeiros^{2

3}, Marcelo A Comini², Mariela Bollati-Fogolín¹

Affiliations

¹ Cell Biology Unit, Institut Pasteur Montevideo, Montevideo, Uruguay.
² Redox Biology of Trypanosomes Lab, Institut Pasteur de Montevideo, Montevideo, Uruguay.
³ Department of Biochemistry, Faculty of Medicine, University of the Republic, Montevideo, Uruguay.

Abstract

Chagas disease (CD) is a life-threatening illness caused by the parasite Trypanosoma cruzi (T. cruzi). With around seven million people infected worldwide and over 50,000 deaths per year, CD is a major public health issue in Latin America. The main route of transmission to humans is through a triatomine bug (vector-borne), but congenital and oral transmission have also been reported. The acute phase of CD presents mild symptoms but may develop into a long-lasting chronic illness, characterized by severely impaired cardiac, digestive, and neurological functions. The intestinal tissue appears to have a key role during oral transmission and chronic infection of CD. In this immune-privileged reservoir, dormant/quiescent parasites have been suggested to contribute to disease persistence, infection relapse, and treatment failure. However, the interaction between the intestinal epithelium and T. cruzi has not been examined in depth, in part, due to the lack of in vitro models that approximate to the biological and structural complexity of this tissue. Therefore, to understand the role played by the intestinal tissue during transmission and chronic infection, physiological models resembling the organ complexity are needed. Here we addressed this issue by establishing and characterizing adult stem cell-derived colonoid infection models that are clinically relevant for CD. 3D and 2D systems of murine intestinal organoids infected with T. cruzi Dm28c (a highly virulent strain associated with oral outbreaks) were analyzed at different time points by confocal microscopy. T. cruzi was able to invade and replicate in intestinal epithelial primary cells grown as intact organoids (3D) and monolayers (2D). The permissiveness to pathogen infection differed markedly between organoids and cell lines (primate and intestinal human cell lines). So far, this represents the first evidence of the potential that these cellular systems offer for the study of host-pathogen interactions and the discovery of effective anti-chagasic drugs.

Keywords: Chagas disease; HT-29 cells; Trypanosoma cruzi; intestinal organoids; murine colon organoids.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Chagas Disease* / parasitology
Colon
Humans
Intestinal Mucosa
Mice
Organoids
Persistent Infection
Trypanosoma cruzi*

Grants and funding

This project was funded by ANII (PhD fellowship, FMV_1_2019_1_156213 and EQL_2013_X_1_2), ACIP grant (ACIP 532-22) from Institut Pasteur Paris, and FOCEM (MERCOSUR Structural Convergence Fund), COF 03/11. HD and CQ received a fellowship from Sistema Nacional de Becas, ANII. AM, MAC, MB-F and RP are members of the SNI (National Research System, Uruguay) and PEDECIBA.