Immunosenescence: what does it mean to health outcomes in older adults?

Abstract

The most profound consequences of immune senescence with respect to human health are the increased susceptibility to infectious diseases and decreased vaccine efficacy. Changes in both innate and adaptive immune function converge in the reduced response to vaccination and protection against infection and related diseases. The decline in thymic output of naïve T cells diminishes responses to novel antigens, such as West Nile Virus, while clonal expansions leading to defects in the T cell repertoire are associated with blunted responses of memory T cells to conserved epitopes of the influenza virus. Recent studies on how immunologic mechanisms of protection change during aging have led to novel strategies for improving vaccine responsiveness and outcomes of infectious diseases in older adults.

Figures

Figure 1

Differentiation from naïve (CD28+CD45RA+) to memory T cells (CD28+CD45RA-), which after several rounds of expansion and contraction of CTL (CD8+ T cells) become terminally differentiated (TEMRA, CD28-CD45RA+).

Figure 2

Generation of antibodies and memory T helper (Th) and cytotoxic T lymphocytes (CTL) in the lymph node in response to influenza vaccination (upper left). Outcome of influenza infection in cells of the respiratory tract (lower right) depends on Th1 vs. Th2 responses to vaccination and activation of CTL-mediated killing of virus-infected cells (Box 1).