High frequency of circulating γδ T cells with dominance of the Vδ1 subset in a healthy population

Abstract

TCR γδ⁺ cells constitute δ1⁺ cells constitute a minority of these cells. In contrast to TCR αβ⁺ cells, their repertoire is selected extrathymically by environmental antigens. Although increased frequencies of V_δ1⁺ cells are found in several diseases, their function remains obscure. Here we show that the frequency of peripheral blood γδ T cells in healthy West Africans is about twice that of Caucasians, mainly due to a 5-fold increase in V_δ1⁺ cells, which is consequently the dominant subset. No age dependency of V_δ1 frequencies was identified and the V_δ1⁺ cells in the African donors did not show preferential V_γ chain usage. Analysis of the CDR3 region size did not reveal any particular skewing of the V_δ1 repertoire, although oligoclonality was more pronounced in adults compared to children. The proportions of CD8⁺, CD38⁺ and CD45RA^hiCD45RO^– cells within the V_δ1⁺ subset were higher in the African than in the European donors, without obvious differences in expression of activation markers. No significant correlations between levels of V_δ1⁺ cells and environmental antigens or immunological parameters were identified. Taken together, the evidence argues against a CDR3-restricted, antigen-driven expansion of V_δ1⁺ cells in the African study population. Our study shows that high frequencies of TCR γδ⁺ cells with dominance of the V_δ1⁺ subset can occur at the population level in healthy people, raising questions about the physiological role of V_δ1⁺ T cells in the function and regulation of the immune system.