AUTHOR=Vietzen Hannes , Staber Philipp B. , Berger Sarah M. , Furlano Philippe L. , Kühner Laura M. , Lubowitzki Simone , Pichler Alexander , Strassl Robert , Cornelissen Jan J. , Puchhammer-Stöckl Elisabeth 

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

JOURNAL=Frontiers in Immunology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2023.1183788

DOI=10.3389/fimmu.2023.1183788

ISSN=1664-3224

ABSTRACT=<p>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<sup>+</sup> Hodgkin (EBV<sup>+</sup>HL) or non-Hodgkin lymphomas (EBV<sup>+</sup>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<sup>+</sup>HL and EBV<sup>+</sup>nHL. Therefore, we recruited a study cohort of 63 EBV<sup>+</sup>HL and EBV<sup>+</sup>nHL patients and 192 controls with confirmed EBV reactivations, but without lymphomas. Here, we demonstrate that in EBV<sup>+</sup> lymphoma patients exclusively the high-affine <italic>LMP-1 GGDPHLPTL</italic> peptide variant-encoding EBV-strains reactivate. In EBV<sup>+</sup>HL and EBV<sup>+</sup>nHL patients, the high-expressing HLA-E*0103/0103 genetic variant was significantly overrepresented. Combined, the LMP-1 <italic>GGDPHLPTL</italic> and HLA-E*0103/0103 variants efficiently inhibited NKG2A+ NK cells, thereby facilitating the <italic>in vitro</italic> spread of EBV-infected tumor cells. In addition, EBV<sup>+</sup>HL and EBV<sup>+</sup>nHL patients, showed impaired pro-inflammatory NKG2C<sup>+</sup> NK cell responses, which accelerated the <italic>in vitro</italic> 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<sup>+</sup>NKG2C<sup>+</sup> NK cells. Thus, the HLA-E/<italic>LMP-1/</italic>NKG2A pathway and individual NKG2C<sup>+</sup> NK cell responses are associated with the progression toward EBV<sup>+</sup> lymphomas.</p>