ABSTRACT: Gamma delta (??) T-cell based immunotherapy is a promising concept for the treatment of hematologic malignancies. Not only in vitro but also in early phase clinical trials, zoledronic acid (Zol) and interleukin-2 (IL-2) have been successfully used to activate human ?? T-cells and to induce clinical anti-tumor effects. Aiming to improve the effectiveness of future ?? T-cell based immunotherapies against leukemia, we analyzed the impact of programmed cell death protein 1 (PD-1) signaling, on the different phases of ?? T-cell activation, of proliferation, production of anti-tumor cytokines and cytotoxic function in vitro. PD-1 expression was found significantly upregulated between day 2 and day 4 following stimulation with Zol and IL-2. However, proliferation or expression of activation markers of ??, ?? and NK-cells are not altered by additional PD-1 blockade. Pembrolizumab increases interferon-? (IFN-?) production in ?? T-cells upon direct stimulation with Zol and in response to Zol treated primary acute myeloid leukemia (AML) cells by approximately 57% and 30%, respectively. Zol sensitized primary AML cells also induce PD-1 expression in co-cultured ?? T-cells and such PD-1(+) cells contain more IFN-?. In contrast, PD-1 blockade does not have a significant effect on direct cell dependent lysis of leukemia cells by ?? T-cells. This study demonstrates that PD-1 blockade impacts cell dependent cytotoxicity and cytokine production in response to leukemia cells differently. While Pembrolizumab did not increase cell lysis of stimulated and expanded ?? T-cells, it induces significant upregulation of the potent pro-inflammatory and anti-tumor cytokine IFN-?, which might facilitate anti-leukemia effects.