[HTML][HTML] Direct and indirect effects of cytomegalovirus-induced γδ T cells after kidney transplantation
L Couzi, V Pitard, JF Moreau, P Merville… - Frontiers in …, 2015 - frontiersin.org
L Couzi, V Pitard, JF Moreau, P Merville, J Déchanet-Merville
Frontiers in immunology, 2015•frontiersin.orgDespite effective anti-viral therapies, cytomegalovirus (CMV) is still associated with direct
(CMV disease) and indirect effects (rejection and poor graft survival) in kidney transplant
recipients. Recently, an unconventional T cell population (collectively designated as Vδ2
neg γδ T cells) has been characterized during the anti-CMV immune response in all solid-
organ and bone-marrow transplant recipients, neonates, and healthy people. These CMV-
induced Vδ2 neg γδ T cells undergo a dramatic and stable expansion after CMV infection, in …
(CMV disease) and indirect effects (rejection and poor graft survival) in kidney transplant
recipients. Recently, an unconventional T cell population (collectively designated as Vδ2
neg γδ T cells) has been characterized during the anti-CMV immune response in all solid-
organ and bone-marrow transplant recipients, neonates, and healthy people. These CMV-
induced Vδ2 neg γδ T cells undergo a dramatic and stable expansion after CMV infection, in …
Despite effective anti-viral therapies, cytomegalovirus (CMV) is still associated with direct (CMV disease) and indirect effects (rejection and poor graft survival) in kidney transplant recipients. Recently, an unconventional T cell population (collectively designated as Vδ2neg γδ T cells) has been characterized during the anti-CMV immune response in all solid-organ and bone-marrow transplant recipients, neonates, and healthy people. These CMV-induced Vδ2neg γδ T cells undergo a dramatic and stable expansion after CMV infection, in a conventional “adaptive” manner. Similarly, as CMV-specific CD8+ αβ T cells, they exhibit an effector/memory TEMRA phenotype and cytotoxic effector functions. Activation of Vδ2neg γδ T cells by CMV-infected cells involves the γδ T cell receptor (TCR) and still ill-defined co-stimulatory molecules such as LFA-1. A multiple of Vδ2neg γδ TCR ligands are apparently recognized on CMV-infected cells, the first one identified being the major histocompatibility complex-related molecule endothelial protein C receptor. A singularity of CMV-induced Vδ2neg γδ T cells is to acquire CD16 expression and to exert an antibody-dependent cell-mediated inhibition on CMV replication, which is controlled by a specific cytokine microenvironment. Beyond the well-demonstrated direct anti-CMV effect of Vδ2neg γδ T cells, unexpected indirect effects of these cells have been also observed in the context of kidney transplantation. CMV-induced Vδ2neg γδ T cells have been involved in surveillance of malignancy subsequent to long-term immunosuppression. Moreover, CMV-induced CD16+ γδ T cells are cell effectors of antibody-mediated rejection of kidney transplants, and represent a new physiopathological contribution to the well-known association between CMV infection and poor graft survival. All these basic and clinical studies paved the road to the development of a future γδ T cell-based immunotherapy. In the meantime, γδ T cell monitoring should prove a valuable immunological biomarker in the management of CMV infection.
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