| Literature DB >> 25100508 |
Nupur Bhatnagar1, Fareed Ahmad, Henoch S Hong, Johanna Eberhard, I-Na Lu, Matthias Ballmaier, Reinhold E Schmidt, Roland Jacobs, Dirk Meyer-Olson.
Abstract
Monocytes are known to engage in reciprocal crosstalk with NK cells but their influence on NK-cell-associated antibody-dependent cellular cytotoxicity (ADCC) is not well understood. We demonstrate that in humans FcγRIII (CD16)-dependent ADCC by NK cells is considerably enhanced by monocytes, and that this effect is regulated by FcγRII (CD32) crosslinking in healthy individuals. It is known that during HIV-1 infection, NK cells are known to express low levels of CD16 and exhibit reduced ADCC. We show that immune regulation of CD16-mediated NK-cell cytotoxicity by monocytes through CD32 engagement is substantially disturbed in chronic progressive HIV-1 infection. Expression of activating isoform of CD32 represented a compensatory mechanism for reduced expression of CD16 on NK cells during HIV-1 infection. As a result, the regulation of NK-cell-associated ADCC by monocytes is skewed and eventually constitutes a novel factor that contributes to HIV-1-associated immune deficiency, dysregulation and pathogenesis. Our data therefore provide evidence, for the first time, that in humans monocytes act as a rheostat for FcγRIII-mediated NK-cell functions maintaining a well-balanced immune response.Entities:
Keywords: ADCC; Fcγ receptors; Monocytes; NK cells
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Year: 2014 PMID: 25100508 DOI: 10.1002/eji.201444515
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532