Long-term growth arrest of PUVA-treated fibroblasts in G2/M in the absence of p16[sup INK4a] , p21[sup CIP1] or p53.

Abstract: Premature aging of the skin is a prominent side-effect of psoralen photoactivation, a therapy used for different skin disorders. Recently, we demonstrated that treatment of fibroblasts with 8-methoxypsoralen and ultraviolet A irradiation resulted in growth arrest with morphological and functional changes reminiscent of replicative senescence. To further elucidate the underlying molecular mechanisms, we analysed the cell-cycle phases of the growth-arrested fibroblasts. After PUVA treatment, fibroblasts arrested in G2/M, in contrast to spontaneously senesced fibroblasts arresting in a cell-cycle phase with many features similar to G1. To address the role of the cell-cycle controlling genes p16[sup INK4a] , p21[sup CIP1] and p53, we analysed the expression of these genes. p16[sup INK4a] , p21[sup CIP1] and p53 protein levels increased substantially with different time kinetics in growth-arrested fibroblasts. Because p16[sup INK4a] , p21[sup CIP1] and p53 are involved in replicative senescence, we applied the PUVA regimen to fibroblasts deficient in either of these genes. p16[sup INK4a] , p21[sup CIP1] and p53 null mutant fibroblast strains underwent growth arrest with a senescent phenotype similar to wild-type human fibroblasts. Based on these results, we propose that redundant or alternate pathways are involved in the response of dermal fibroblasts to PUVA treatment resulting in a phenocopy of replicative senescence in vitro . [ABSTRACT FROM AUTHOR]