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Departamento de Inmunología y Oncología, Centro Nacional de Biotecnología, Universidad Autónoma de Madrid, Cantoblanco, Madrid, Spain
Developing T cells journey through the different thymic
microenvironments while receiving signals that eventually will allow
some of them to become mature naive T cells exported to the periphery.
This maturation can be visualized by the phenotype of the developing
cells. CCR8 is a
-chemokine receptor preferentially expressed in the
thymus. We have developed 8F4, an anti-mouse CCR8 mAb that is able
to neutralize the ligand-induced activation of CCR8, and used it to
characterize the CCR8 protein expression in the different thymocyte
subsets. Taking into account the intrathymic lineage relationships, our
data showed that CCR8 expression in thymus followed two transient waves
along T cell maturation. The first one took place in CD4-
CD8- double-negative thymocytes, which showed a low CCR8
expression, and the second wave occurred after TCR activation by the
Ag-dependent positive selection in CD4+ CD8+
double-positive cells. From that maturation stage, CCR8 expression
gradually increased as the CD4+ cell differentiation
proceeded, reaching a maximum at the CD4+ CD8-
single-positive stage. These CD4+ cells expressing CCR8
were also CD69high CD62Llow thymocytes,
suggesting that they still needed to undergo some differentiation step
before becoming functionally competent naive T cells ready to be
exported from the thymus. Interestingly, no significant amounts of CCR8
protein were detectable in CD4- CD8+
thymocytes. Our data showing a clear regulation of the CCR8 protein in
thymus suggest a relevant role for CCR8 in this lymphoid organ, and
identify CCR8 as a possible marker of thymocyte subsets recently
committed to the CD4+ lineage.
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