CD4+CD8+(thymocyte-like) T lymphocytes present in blood and skin from patients with atopic dermatitis suggest immune dysregulation

Background Atopic dermatitis (AD) is a chronic inflammatory skin disease ex pressed early in life. Disease development is primarily determined by as ye t unknown genetic factors, leading to the accumulation of activated T lymph ocytes in the skin. Objectives To investigate the nature of these T cells. Methods T-cell lines could be established from AD skin biopsies, but not fr om normal skin or AD peripheral blood, when placed in RPMI 1640 medium with 10% human AB serum, antibiotics, and the T-lymphocyte growth factors inter leukins 2 and 4. The cell lines were subjected to phenotypic analysis using a fluorescence-activated cell sorter and compared with lymphocytes from AD and normal control peripheral blood. Results T-cell lines from 22 of 24 consecutive skin biopsies taken from 24 adult patients with AD were established. All cells were T lymphocytes expre ssing several activation markers. A significant proportion of the lymphocyt es had stable expression of a CD4+ CD8+ phenotype (26% +/- 6%; mean +/- SEM ). Such double-positive T lymphocytes are normally only seen in the thymus and not in the peripheral immune system. CD4+ CD8+ cells in peripheral bloo d of the patients (12.5% +/- 3.3%) were also detected. Conclusions We suggest that a basic pathophysiological change in AD may be a faulty maturation of the T-lymphocyte system, leading to skin inflammatio n with CD4+ CD8+ T lymphocytes resembling immature T cells. This is likely to lead to skewing of many immune reactions in the patients.