[PDF][PDF] Memory inflation during chronic viral infection is maintained by continuous production of short-lived, functional T cells

CM Snyder, KS Cho, EL Bonnett, S van Dommelen… - Immunity, 2008 - cell.com
CM Snyder, KS Cho, EL Bonnett, S van Dommelen, GR Shellam, AB Hill
Immunity, 2008cell.com
During persistent murine cytomegalovirus (MCMV) infection, the T cell response is
maintained at extremely high intensity for the life of the host. These cells closely resemble
human CMV-specific cells, which compose a major component of the peripheral T cell
compartment in most people. Despite a phenotype that suggests extensive antigen-driven
differentiation, MCMV-specific T cells remain functional and respond vigorously to viral
challenge. We hypothesized that a low rate of antigen-driven proliferation would account for …
Summary
During persistent murine cytomegalovirus (MCMV) infection, the T cell response is maintained at extremely high intensity for the life of the host. These cells closely resemble human CMV-specific cells, which compose a major component of the peripheral T cell compartment in most people. Despite a phenotype that suggests extensive antigen-driven differentiation, MCMV-specific T cells remain functional and respond vigorously to viral challenge. We hypothesized that a low rate of antigen-driven proliferation would account for the maintenance of this population. Instead, we found that most of these cells divided only sporadically in chronically infected hosts and had a short half-life in circulation. The overall population was supported, at least in part, by memory T cells primed early in infection, as well as by recruitment of naive T cells at late times. Thus, these data show that memory inflation is maintained by a continuous replacement of short-lived, functional cells during chronic MCMV infection.
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