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Inhibitory NKG2A+ and absent activating NKG2C+ NK cell responses are associated with the development of EBV+ lymphomas

Hannes Vietzen, Philipp B. Staber, S. Berger, Philippe L. Furlano, Laura M. Kühner, Simone Lubowitzki, Alexander Pichler, Robert Straßl, Jan J. Cornelissen, Elisabeth Puchhammer‐Stöckl

2023Frontiers in Immunology16 citationsDOIOpen Access PDF

Abstract

Epstein-Barr virus (EBV) is a ubiquitous herpesvirus, which infects over 90% of the adult human population worldwide. After primary infections, EBV is recurrently reactivating in most adult individuals. It is, however, unclear, why these EBV reactivations progress to EBV + Hodgkin (EBV + HL) or non-Hodgkin lymphomas (EBV + nHL) only in a minority of EBV-infected individuals. The EBV LMP-1 protein encodes for a highly polymorphic peptide, which upregulates the immunomodulatory HLA-E in EBV-infected cells, thereby stimulating the inhibitory NKG2A-, but also the activating NKG2C-receptor on natural killer (NK) cells. Using a genetic-association approach and functional NK cell analyses, we now investigated, whether these HLA-E-restricted immune responses impact the development of EBV + HL and EBV + nHL. Therefore, we recruited a study cohort of 63 EBV + HL and EBV + nHL patients and 192 controls with confirmed EBV reactivations, but without lymphomas. Here, we demonstrate that in EBV + lymphoma patients exclusively the high-affine LMP-1 GGDPHLPTL peptide variant-encoding EBV-strains reactivate. In EBV + HL and EBV + nHL patients, the high-expressing HLA-E*0103/0103 genetic variant was significantly overrepresented. Combined, the LMP-1 GGDPHLPTL and HLA-E*0103/0103 variants efficiently inhibited NKG2A+ NK cells, thereby facilitating the in vitro spread of EBV-infected tumor cells. In addition, EBV + HL and EBV + nHL patients, showed impaired pro-inflammatory NKG2C + NK cell responses, which accelerated the in vitro EBV-infected tumor cells spread. In contrast, the blocking of NKG2A by monoclonal antibodies (Monalizumab) resulted in efficient control of EBV-infected tumor cell growth, especially by NKG2A + NKG2C + NK cells. Thus, the HLA-E/ LMP-1/ NKG2A pathway and individual NKG2C + NK cell responses are associated with the progression toward EBV + lymphomas.

Topics & Concepts

ImmunologyEpstein–Barr virusLymphomaBiologyImmune systemVirusAntibodyVirologyMonoclonal antibodyCancer researchImmune Cell Function and InteractionViral-associated cancers and disordersLymphoma Diagnosis and Treatment
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