Distinct Features of Canine Non-conventional CD4(−)CD8α(−) Double-Negative TCRαβ(+) vs. TCRγδ(+) T Cells

The role of conventional TCRαβ(+)CD4(+) or TCRαβ(+)CD8α(+) single-positive (sp) T lymphocytes in adaptive immunity is well-recognized. However, non-conventional T cells expressing TCRαβ or TCRγδ but lacking CD4 and CD8α expression [i.e., CD4(−)CD8α(−) double-negative (dn) T cells] are thought to pla...

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Detalles Bibliográficos
Autores principales: Rabiger, Friederike V., Rothe, Kathrin, von Buttlar, Heiner, Bismarck, Doris, Büttner, Mathias, Moore, Peter F., Eschke, Maria, Alber, Gottfried
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6883510/
https://www.ncbi.nlm.nih.gov/pubmed/31824515
http://dx.doi.org/10.3389/fimmu.2019.02748
Descripción
Sumario:The role of conventional TCRαβ(+)CD4(+) or TCRαβ(+)CD8α(+) single-positive (sp) T lymphocytes in adaptive immunity is well-recognized. However, non-conventional T cells expressing TCRαβ or TCRγδ but lacking CD4 and CD8α expression [i.e., CD4(−)CD8α(−) double-negative (dn) T cells] are thought to play a role at the interface between the innate and adaptive immune system. Dn T cells are frequent in swine, cattle or sheep and predominantly express TCRγδ. In contrast, TCRγδ(+) T cells are rare in dogs. In this study, we identified a high proportion of canine dn T cells in the TCRαβ(+) T cell population of PBMC, lymphatic and non-lymphatic organs. In PBMC, the frequency of this T cell subpopulation made up one third of the frequency of TCRαβ(+)CD4(+) sp, and almost half of the frequency of TCRαβ(+)CD8α(+) sp T cells (i.e., ~15% of all TCRαβ(+) T cells). Among TCRαβ(+)CD4(−)CD8α(−) dn T cells of PBMC and tissues, FoxP3(+) cells were identified indicating regulatory potential of this T cell subset. 80% of peripheral blood FoxP3(+)TCRαβ(+)CD4(−)CD8α(−) dn T cells co-expressed CD25, and, interestingly, also the FoxP3-negative TCRαβ(+)CD4(−)CD8α(−) dn T cells comprised ~34% CD25(+) cells. Some of the FoxP3-positive TCRαβ(+)CD4(−)CD8α(−) dn T cells co-expressed GATA-3 suggesting stable function of regulatory T cells. The frequency of GATA-3 expression by FoxP3(−)TCRαβ(+)CD4(−)CD8α(−) dn T cells was even higher as compared with TCRαβ(+)CD4(+) sp T cells (20.6% vs. 11.9%). Albeit lacking FoxP3 and CD25 expression, TCRγδ(+)CD4(−)CD8α(−) dn T cells also expressed substantial proportions of GATA-3. In addition, TCRαβ(+)CD4(−)CD8α(−) dn T cells produced IFN-γ and IL-17A upon stimulation. T-bet and granzyme B were only weakly expressed by both dn T cell subsets. In conclusion, this study identifies two dn T cell subsets in the dog: (i) a large (~7.5% in Peyer's patches, ~15% in lung) population of TCRαβ(+)CD4(−)CD8α(−) dn T cells with subpopulations thereof showing an activated phenotype, high expression of FoxP3 or GATA-3 as well as production of IFN-γ or IL-17A and (ii) a small TCRγδ(+)CD4(−)CD8α(−) dn T cell subset also expressing GATA-3 without production of IFN-γ or IL-17A. It will be exciting to unravel the function of each subset during immune homeostasis and diseases of dogs.

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