Abstract

BackgroundIn many virus infections natural killer (NK) cells are critical for the rapid containment of virus replication. Polymorphisms in NK cell receptors as well as viral escape from NK cell responses are associated with pathogenesis and viral loads in HIV-infected individuals, emphasizing their importance in retroviral immunity. In contrast, NK cells of LCMV-infected mice dampened virus-specific T cell responses resulting in impaired virus control. Thus, the exact role of NK cells during different phases of viral infections remains elusive. In this study we characterized the NK cell response at different time points of an acute retroviral infection by using the Friend retrovirus (FV) mouse model.FindingsDepletion of NK1.1+ cells during the initial phase of FV infection (3 to 4 days post infection) resulted in increased viral loads, which correlated with enhanced target cell killing and elevated NK cell effector functions. At days 7 to 15 post infection, NK and NKT cells did not contribute to anti-retroviral immunity. In the transition phase between acute and chronic infection (30 days post infection), NK and NKT cells exhibited an inhibitory role and their depletion resulted in reduced viral loads and significantly improved FV-specific CD8+ T cell responses.ConclusionsOur results demonstrate an opposed activity of NK cells during retroviral infection. They were protective in the initial phase of infection, when adaptive T cell responses were not yet detectable, but were dispensable for viral immunity after T cell expansion. At later time points they exhibited regulatory functions in inhibiting virus-specific CD8+ T cell responses.

Highlights

  • In many virus infections natural killer (NK) cells are critical for the rapid containment of virus replication

  • NK cells are cytotoxic cells of the innate immune system, which contribute to the control of many virus infections

  • For several viral infections it was shown that NK cells suppress the adaptive immunity by killing virus–specific T cells [1,2,3,4]

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Summary

Introduction

In many virus infections natural killer (NK) cells are critical for the rapid containment of virus replication. At this early time point of infection no significant activation of NK and NKT cells, indicated by the expression of CD69, was found (Figure 3A, 3B and data not shown).

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