Pathogens (Aug 2020)

After Experimental <i>Trypanosoma cruzi</i> Infection, Dying Hepatic CD3<sup>+</sup>TCRαβ<sup>+</sup>B220<sup>+</sup> T Lymphocytes Are Rescued from Death by Peripheral T Cells and Become Activated

  • Natalia Vacani-Martins,
  • Marcelo Meuser-Batista,
  • Otacilio C. Moreira,
  • Cynthia Machado Cascabulho,
  • Daniela Gois Beghini,
  • Samuel Iwao Horita,
  • Marcos Meuser Batista,
  • Fernando Cleber Freitas,
  • Juliana Rodrigues Guimarães,
  • Andrea Henriques-Pons

DOI
https://doi.org/10.3390/pathogens9090717
Journal volume & issue
Vol. 9, no. 9
p. 717

Abstract

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The unusual phenotype of CD3+ T lymphocyte expressing B220, a marker originally attributed to B lymphocytes, was first observed in the liver of Fas/Fas-L-deficient mice as a marker of apoptotic T lymphocytes. However, other CD3+B220+ T lymphocyte populations were later described in the periphery as functional cytotoxic or regulatory cells, for example. Then, in this work, we studied whether hepatic CD3+B220+ T lymphocytes could play a role in experimental Trypanosoma cruzi infection. In control and infected mice, we observed two subpopulations that could be discerned based on CD117 expression, which were conventional apoptotic CD3+B220+(CD117−) and thymus-independent CD3+B220+CD117+ T lymphocytes. Regardless of CD117 expression, most B220+ T lymphocytes were 7AAD+, confirming this molecule as a marker of dying T cells. However, after infection, we found that around 15% of the CD3+B220+CD117+ hepatic population became B220 and 7AAD negative, turned into CD90.2+, and upregulated the expression of CD44, CD49d, and CD11a, a phenotype consistent with activated T lymphocytes. Moreover, we observed that the hepatic CD3+B220+CD117+ population was rescued from death by previously activated peripheral T lymphocytes. Our results extend the comprehension of the hepatic CD3+B220+ T lymphocyte subpopulations and illustrate the complex interactions that occur in the liver.

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