| Literature DB >> 28704647 |
Christian Körner1, Camille R Simoneau2, Philipp Schommers3, Mitchell Granoff2, Maja Ziegler4, Angelique Hölzemer5, Sebastian Lunemann4, Janet Chukwukelu6, Björn Corleis2, Vivek Naranbhai7, Douglas S Kwon8, Eileen P Scully9, Stephanie Jost10, Frank Kirchhoff11, Mary Carrington7, Marcus Altfeld4.
Abstract
It was widely accepted that HIV-1 downregulates HLA-A/B to avoid CTL recognition while leaving HLA-C unaltered in order to prevent NK cell activation by engaging inhibitory NK cell receptors, but it was recently observed that most primary isolates of HIV-1 can mediate HLA-C downmodulation. Now we report that HIV-1-mediated downmodulation of HLA-C was associated with reduced binding to its respective inhibitory receptors. Despite this, HLA-C-licensed NK cells displayed reduced antiviral activity compared to their unlicensed counterparts, potentially due to residual binding to the respective inhibitory receptors. Nevertheless, NK cells were able to sense alterations of HLA-C expression demonstrated by increased antiviral activity when exposed to viral strains with differential abilities to downmodulate HLA-C. These results suggest that the capability of HLA-C-licensed NK cells to control HIV-1 replication is determined by the strength of KIR/HLA-C interactions and is thus dependent on both host genetics and the extent of virus-mediated HLA-C downregulation.Entities:
Keywords: HIV-1; HLA class I; HLA-C; KIR; NK cells; natural killer cells
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Year: 2017 PMID: 28704647 PMCID: PMC5565794 DOI: 10.1016/j.chom.2017.06.008
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023