Signaling pathways in aged T cells - A reflection of T cell differentiation, cell senescence and host environment SEMINARS IN IMMUNOLOGY Goronzy, J. J., Li, G., Yu, M., Weyand, C. M. 2012; 24 (5): 365-372

Abstract

With increasing age, the ability of the immune system to protect against new antigenic challenges or to control chronic infections erodes. Decline in thymic function and cumulating antigenic experiences of acute and chronic infections threaten T cell homeostasis, but insufficiently explain the failing immune competence and the increased susceptibility for autoimmunity. Alterations in signaling pathways in the aging T cells account for many of the age-related defects. Signaling threshold calibrations seen with aging frequently built on mechanisms that are operational in T cell development and T cell differentiation or are adaptations to the changing environment in the aging host. Age-related changes in transcription of receptors and signaling molecules shift the balance towards inhibitory pathways, most dominantly seen in CD8 T cells and to a lesser degree in CD4 T cells. Prominent examples are the expression of negative regulatory receptors of the CD28 and the TNF receptor superfamilies as well the expression of various cytoplasmic and nuclear dual-specific phosphatases.

View details for DOI 10.1016/j.smim.2012.04.003

View details for Web of Science ID 000311017700009

View details for PubMedID 22560928

View details for PubMedCentralID PMC3435478