1. Spatiotemporal trafficking of HIV in human plasmacytoid dendritic cells defines a persistently IFN-α-producing and partially matured phenotype
- Author
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O'Brien, Meagan, Manches, Olivier, Sabado, Rachel Lubong, Baranda, Sonia Jimenez, Wang, Yaming, Marie, Isabelle, Rolnitzky, Linda, Markowitz, Martin, Margolis, David M., Levy, David, and Bhardwaj, Nina
- Subjects
HIV (Viruses) -- Genetic aspects -- Health aspects -- Research ,Interferon alpha -- Physiological aspects -- Research ,Dendritic cells -- Physiological aspects -- Research ,Health care industry - Abstract
Plasmacytoid DCs (pDCs) are innate immune cells that are specialized to produce IFN-α and to activate adaptive immune responses. Although IFN-α inhibits HIV-1 replication in vitro, the production of IFN-α by HIV activated pDCs in vivo may contribute more to HIV pathogenesis than to protection. We have now shown that HIV-stimulated human pDCs allow for persistent IFN-α production upon repeated stimulation, express low levels of maturation molecules, and stimulate weak T cell responses. Persistent IFN-α production by HIV-stimulated pDCs correlated with increased levels of IRF7 and was dependent upon the autocrine IFN-α/β receptor feedback loop. Because it has been shown that early endosomal trafficking of TLR9 agonists causes strong activation of the IFN-α pathway but weak activation of the NF-κB pathway, we sought to investigate whether early endosomal trafficking of HIV, a TLR7 agonist, leads to the IFN-α-producing phenotype we observed. We demonstrated that HIV preferentially traffics to the early endosome in human pDCs and therefore skews pDCs toward a partially matured, persistently IFN-α-secreting phenotype., Introduction Plasmacytoid DCs (pDCs) are innate immune cells that circulate in the blood and lymphoid tissues and are specialized to produce copious amounts of type I IFNs (IFN-α/β) in response [...]
- Published
- 2011
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