Requirement of Species-Specific Interactions for the Activation of Human γδ T Cells by Pamidronate

Abstract

Human γδ T cells bearing Vγ2Vδ2-TCR recognize various kinds of small nonpeptide Ags, and activation of them by a nitrogen-containing bisphosphonate Ag, pamidronate, requires Ag presentation by cells other than γδ T cells, including many human tumor cells. Present results demonstrated that tumor cell lines of nonhuman origins pulsed with pamidronate failed to activate human γδ T cells without exception, whereas most if not all human tumor cell lines could do so. γδ T cells formed stable conjugates with pamidronate-pulsed human tumor cells and both conjugate formation and γδ T cell activation were inhibited significantly by anti-LFA-1 mAb, suggesting the requirement of LFA-1-mediated interaction with APC for efficient γδ T cell activation. Consistently, ICAM-1^low tumor cell lines pulsed with pamidronate induced no or only weak activation of γδ T cells, whereas similarly treated ICAM-1^high cell lines could activate them. One of the two ICAM-1^low tumor cell lines pulsed with pamidronate induced strong γδ T cell activation after ICAM-1 gene transfer. However, another ICAM-1^low human cell line as well as murine tumor cell lines pulsed with pamidronate remained totally defective in γδ T cell activation even after expression of human ICAM-1. These results suggested that activation of human γδ T cells by nonpeptide Ags required species-specific interactions in addition to LFA-1/ICAM-1-mediated cell adhesion with APC.