International Journal of Molecular Sciences (Dec 2021)

<i>Mycobacterium tuberculosis</i> H37Rv Strain Increases the Frequency of CD3<sup>+</sup>TCR<sup>+</sup> Macrophages and Affects Their Phenotype, but Not Their Migration Ability

  • Lucero A. Ramon-Luing,
  • Claudia Carranza,
  • Norma A. Téllez-Navarrete,
  • Karen Medina-Quero,
  • Yolanda Gonzalez,
  • Martha Torres,
  • Leslie Chavez-Galan

DOI
https://doi.org/10.3390/ijms23010329
Journal volume & issue
Vol. 23, no. 1
p. 329

Abstract

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In mycobacterial infections, the number of cells from two newly discovered subpopulations of CD3+ myeloid cells are increased at the infection site; one type expresses the T cell receptor (CD3+TCRαβ+) and the other does not (CD3+TCRαβ−). The role of Mycobacterium tuberculosis (Mtb) virulence in generating these subpopulations and the ability of these cells to migrate remains unclear. In this study, monocyte-derived macrophages (MDMs) infected in vitro with either a virulent (H37Rv) or an avirulent (H37Ra) Mtb strain were phenotypically characterized based on three MDM phenotypes (CD3−, CD3+TCRαβ+, and CD3+TCRαβ−); then, their migration ability upon Mtb infection was evaluated. We found no differences in the frequency of CD3+ MDMs at 24 h of infection with either Mtb strain. However, H37Rv infection increased the frequency of CD3+TCRαβ+ MDMs at a multiplicity of infection of 1 and altered the expression of CD1b, CD1c, and TNF on the surface of cells from both the CD3+ MDM subpopulations; it also modified the expression of CCR2, CXCR1, and CCR7, thus affecting CCL2 and IL-8 levels. Moreover, H37Rv infection decreased the migration ability of the CD3− MDMs, but not CD3+ MDMs. These results confirm that the CD3+ macrophage subpopulations express chemokine receptors that respond to chemoattractants, facilitating cell migration. Together, these data suggest that CD3+ MDMs are a functional subpopulation involved in the immune response against Mtb.

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