AUTHOR=Vollmers Sarah , Lobermeyer Annabelle , Niehrs Annika , Fittje Pia , Indenbirken Daniela , Nakel Jacqueline , Virdi Sanamjeet , Brias Sebastien , Trenkner Timo , Sauer Gabriel , Peine Sven , Behrens Georg M.N. , Lehmann Clara , Meurer Anja , Pauli Ramona , Postel Nils , Roider Julia , Scholten Stefan , Spinner Christoph D. , Stephan Christoph , Wolf Eva , Wyen Christoph , Richert Laura , Norman Paul J. , Sauter Jürgen , Schmidt Alexander H. , Hoelzemer Angelique , Altfeld Marcus , Körner Christian 

TITLE=Host KIR/HLA-C Genotypes Determine HIV-Mediated Changes of the NK Cell Repertoire and Are Associated With Vpu Sequence Variations Impacting Downmodulation of HLA-C

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.922252

DOI=10.3389/fimmu.2022.922252

ISSN=1664-3224

ABSTRACT=<p>NK cells play a pivotal role in viral immunity, utilizing a large array of activating and inhibitory receptors to identify and eliminate virus-infected cells. Killer-cell immunoglobulin-like receptors (KIRs) represent a highly polymorphic receptor family, regulating NK cell activity and determining the ability to recognize target cells. Human leukocyte antigen (HLA) class I molecules serve as the primary ligand for KIRs. Herein, HLA-C stands out as being the dominant ligand for the majority of KIRs. Accumulating evidence indicated that interactions between HLA-C and its inhibitory KIR2DL receptors (KIR2DL1/L2/L3) can drive HIV-1-mediated immune evasion and thus may contribute to the intrinsic control of HIV-1 infection. Of particular interest in this context is the recent observation that HIV-1 is able to adapt to host <italic>HLA-C</italic> genotypes through Vpu-mediated downmodulation of HLA-C. However, our understanding of the complex interplay between <italic>KIR/HLA</italic> immunogenetics, NK cell-mediated immune pressure and HIV-1 immune escape is still limited. Therefore, we investigated the impact of specific <italic>KIR/HLA-C</italic> combinations on the NK cell receptor repertoire and HIV-1 Vpu protein sequence variations of 122 viremic, untreated HIV-1<sup>+</sup> individuals. Compared to 60 HIV-1<sup>-</sup> controls, HIV-1 infection was associated with significant changes within the NK cell receptor repertoire, including reduced percentages of NK cells expressing NKG2A, CD8, and KIR2DS4. In contrast, the NKG2C<sup>+</sup> and KIR3DL2<sup>+</sup> NK cell sub-populations from HIV-1<sup>+</sup> individuals was enlarged compared to HIV-1<sup>-</sup> controls. Stratification along <italic>KIR/HLA-C</italic> genotypes revealed a genotype-dependent expansion of KIR2DL1<sup>+</sup> NK cells that was ultimately associated with increased binding affinities between KIR2DL1 and HLA-C allotypes. Lastly, our data hinted to a preferential selection of Vpu sequence variants that were associated with HLA-C downmodulation in individuals with high KIR2DL/HLA-C binding affinities. Altogether, our study provides evidence that HIV-1-associated changes in the KIR repertoire of NK cells are to some extent predetermined by host <italic>KIR2DL/HLA-C</italic> genotypes. Furthermore, analysis of Vpu sequence polymorphisms indicates that differential KIR2DL/HLA-C binding affinities may serve as an additional mechanism how host genetics impact immune evasion by HIV-1.</p>