Abstract
Beyond midlife, the immune system shows aging features and its defensive capability becomes impaired, by a process known as immunosenescence that involves many changes in the innate and adaptive responses. Innate immunity seems to be better preserved globally, while the adaptive immune response exhibits profound age-dependent modifications. Elderly people display a decline in numbers of naïve T-cells in peripheral blood and lymphoid tissues, while, in contrast, their proportion of highly differentiated effector and memory T-cells, such as the CD28null T-cells, increases markedly. Naïve and memory CD4+ T-cells constitute a highly dynamic system with constant homeostatic and antigen-driven proliferation, influx, and loss of T-cells. Thymic activity dwindles with age and essentially ceases in the later decades of life, severely constraining the generation of new T-cells. Homeostatic control mechanisms are very effective at maintaining a large and diverse subset of naïve CD4+ T-cells throughout life, but although later than in CD8 + T-cell compartment, these mechanisms ultimately fail with age.
Highlights
Throughout life the aging of the immune system causes impairment of its defense capability, in a process known as immunosenescence
EFFECT OF IL-15 HOMEOSTATIC CYTOKINE ON HIGHLY DIFFERENTIATED CD4+ T-CELLS It is widely accepted that IL-7 signaling through the IL-7 receptor (IL-7R), is essential for prolonged survival and proliferation of naïve and memory T-cells
CONCLUDING REMARKS Changes similar to those observed in CD8+ T-cells during aging appear, albeit belatedly, in the compartment of CD4+ Tlymphocytes
Summary
Throughout life the aging of the immune system causes impairment of its defense capability, in a process known as immunosenescence. Any age-associated changes in CD4+ T-cell function including proliferation and cytokine production could be secondary to the alteration in the frequency of naïve and memory T-cells. The accumulation of CD28null T-cells is associated with a reduced overall immune response to pathogens and vaccines in the elderly (Saurwein-Teissl et al, 2002).
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