Dissociated Production of Perforin, Granzyme B, and IFN-γ by HIV-Specific CD8+ Cells in HIV Infection

CD8+ T cells play a crucial role in the control of viral infections such as HIV. The functional characterization of HIV-specific CD8+ T cells has so far been largely restricted to studies of IFN-γ. The TCR-triggered release of the effector molecules perforin (PFN) and granzyme B (GzB), however, is thought to be a central pathway for the destruction of virus-infected target cells by CD8+ effector T cells. Here we would like to address two major findings. On the one hand we propose that ex vivo measurements of PFN and GzB secretion via ELISPOT may permit the distinction between in vivo resting versus activated CD8+ memory T cells in healthy and HIV-infected individuals. Therefore, extending the present standard of IFN-γ measurements to the analysis of PFN and GzB release in functional T cell assays will provide new insights into CD8+ effector T cell functions. It should enable the evaluation of therapeutic vaccination efficacy by its ability to reactivate and convert IFN-γ-positive, but GzB- and PFN-negativ...