| Literature DB >> 33278000 |
L Dold1,2, L Zimmer1, C Schwarze-Zander1,2, C Boesecke1,2, R Mohr1,2, J-C Wasmuth1,2, K Ommer3, B Gathof3, B Krämer1, J Nattermann1,2, C P Strassburg1,2, J K Rockstroh1,2, U Spengler1, B Langhans4,5.
Abstract
HLA-B*57 affects the course of HIV infection. Under antiretroviral therapy, its effects cannot be explained by outstandingly efficient T cell responses alone but may also involve cells of innate immunity. Studying in vitro stimulation with Pam3CSK4, E. coli LPS-B5 and CpG-ODN-2216, we observed greater induction of IL-6/IL-1beta double-positive CD14+CD16++ monocytes as well as IFN-gamma-positive cytotoxic CD56highCD16neg NK cells in HLA-B*57- versus HLA-B*44-positive HIV patients, while TNF-alpha induction remained unchanged. Differences were not seen in the other monocyte and NK cell subsets or in HLA-matched healthy controls. Our findings show that, in virally suppressed HIV infection, HLA-B*57 is associated with enhanced responsiveness of inflammatory innate immune cells to TLR ligands, possibly contributing to increased vulnerability in sepsis. KEY MESSAGES: • HLA-B*57 is a host factor affecting clinical outcomes of HIV infection. • HLA-B*57 modifies inflammatory subsets of NK cells and monocytes in HIV infection. • In HLA-B*57-positive HIV patients TLR agonists induce enhanced IL-6/IL-1beta in monocytes. • NK cells from HLA-B*57 HIV patients release more IFN-gamma upon TLR costimulation. • HLA-B*57 is linked to enhanced inflammatory responsiveness to TLR ligands.Entities:
Keywords: Bacterial infections; HIV; HLA-B*57; Inflammatory immune response; Toll-like receptor stimulation; cART
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Year: 2020 PMID: 33278000 PMCID: PMC7782382 DOI: 10.1007/s00109-020-01996-7
Source DB: PubMed Journal: J Mol Med (Berl) ISSN: 0946-2716 Impact factor: 4.599