Abstract
The aging of the immune system, also named immunosenescence, affects vaccine responses. However, the onset of agerelated immunosenescence has been uncertain, in particularly with regard to vaccine responses. Here, we show that the formation of antibodies in response to vaccination against hepatitis B virus infection was significantly reduced for donors with a mean age of 61 y compared with a group with a mean age of 33 y. Booster vaccination sero-converted the elderly donors, but only at a reduced level, while a stronger response was found for the group of young donors. Agreeing with these findings, the hepatitis B surface antigen-specific proliferative responses by donor-derived T cells were reduced for the elder donors. Interestingly, the association between expression of the adhesion molecule CD62L (L-selectin) on naïve and central memory T cells and the formation of antigen-specific antibodies differed significantly between younger and elder donors. This finding corresponds well with the observation made previously that CD62L gene ablation in animals alters the formation of antigen-specific antibodies. We suggest that a complex interplay between the expression of CD62L and its ligands is a determinant in early-age immunosenescence affecting the response to HBV vaccination. © 2013 Landes Bioscience.
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Rosenberg, C., Bovin, N. V., Bram, L. V., Flyvbjerg, E., Erlandsen, M., Vorup-Jensen, T., & Petersen, E. (2013). Age is an important determinant in humoral and T cell responses to immunization with hepatitis B surface antigen. In Human Vaccines and Immunotherapeutics (Vol. 9, pp. 1466–1476). https://doi.org/10.4161/hv.24480
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