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Review
. 2013 Jan 5;435(1):37-45.
doi: 10.1016/j.virol.2012.10.005.

NK cells controlling virus-specific T cells: Rheostats for acute vs. persistent infections

Raymond M Welsh  1 Stephen N Waggoner
Affiliations
Review

NK cells controlling virus-specific T cells: Rheostats for acute vs. persistent infections

Raymond M Welsh et al. Virology. .

Abstract

Viral infections characteristically induce a cytokine-driven activated natural killer (NK) cell response that precedes an antigen-driven T cell response. These NK cells can restrain some but not all viral infections by attacking virus-infected cells and can thereby provide time for an effective T cell response to mobilize. Recent studies have revealed an additional immunoregulatory role for the NK cells, where they inhibit the size and functionality of the T cell response, regardless of whether the viruses are themselves sensitive to NK cells. This subsequent change in T cell dynamics can alter patterns of immunopathology and persistence and implicates NK cells as rheostat-like regulators of persistent infections.

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Figures

Figure 1
Figure 1. Innate and adaptive host response to infection
This figure portrays the timing of the peaks in innate cytokines (type 1 IFN, etc), NK cell cytolytic activity (not cell number), and T cell number and activity during an acute viral infection, based on (Welsh, 1978).
Figure 2
Figure 2. Pathogenesis of LCMV infection at different viral doses in normal or NK cell-depleted mice
The red area is the zone of severe immune pathology, where there are sufficient amounts of virus and T cells to cause tissue damage. At a higher dose of virus the T cells exhaust, and at a lower dose the virus is cleared. NK cell depletion results in a stronger T cell response, which changes the dose at which immune pathology occurs (Waggoner et al., 2012).
Figure 3
Figure 3. In vivo cytotoxicity assay
Splenocytes from NK cell-depleted, virus-infected Ly5.1+ mice are labeled with CFSE and transferred into infected or uninfected recipients deleted or not of NK cells. After 5 hours donor target cells are gated for CD4 or CD8, and the numbers of cells expressing activation antigens (e.g. CD43 and CD44) are quantified (Waggoner et al., 2012).
Figure 4
Figure 4. NK cells regulate the T cell response by acting on CD4 T cells
This diagrams how NK cells can regulate the overall T cell response by attacking activated helper CD4 T cells. This allows for excess viral antigen that can exhaust both CD4 and CD8 T cells.
See this image and copyright information in PMC

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