Abstract
Background and aim Our research aims to decipher the mechanism and immune consequences imposed by HIV-mediated modulation of autophagy in challenged dendritic cell (DC) subsets, in particular Langerhans cells (LC). Autophagy is an ubiquitous cellular process involved in lysosomalmediated degradation of host components as well as invading pathogens. In previous reports, HIV-1 was shown to modulate the autophagy flux in various immune cell types, including T cells, macrophages and myeloid dendritic cells. However, very little is known about the potential autophagy-driven antiviral activity in LC. Methods LC used for this study were differentiated from either blood monocytes or the MUTZ-3 cell line model which phenotypically mimic LC morphology and immune features. LC were treated with wild type HIV-1, VSV-G pseudotyped HIV-1-derived lentivectors or recombinant HIV-1 envelopes. Levels of infection and cellular autophagy flux were analyzed by western blotting, FACS and confocal imaging. Results We observe that, as previously described for myeloid DC, autophagy flux is compromised in LC after exposure to HIV-1 envelope or infectious virus. Hence, activation of the autophagy negative regulator, mTOR, is detected, and could account for the autophagy flux inhibition. Although we could confirm the HIV-1 restriction activity of langerin and SAMHD-1 in LC, it appears that shutting down autophagy flux is an early cellular target for the virus thus strongly suggesting that it might be involved in HIV-1 clearance shortly upon viral entry. Conclusion In this study, we show that Langerin and SAMHD-1 are significantly restricting HIV-1 entry and replication in LC. However, an additional barrier to infection, such as autophagolysosome-mediated degradation of virus particles, may account for the low infection rate observed in LC. Our results suggest that autophagy flux is indeed dampened upon HIV-1 challenge which might favour virus progression. We further aim to examine the effect of autophagy modulation on virus infection of LC and consequent virus transmission to CD4 + T cells.
Highlights
Background and aimOur research aims to decipher the mechanism and immune consequences imposed by HIV-mediated modulation of autophagy in challenged dendritic cell (DC) subsets, in particular Langerhans cells (LC)
In this study, we show that Langerin and SAMHD-1 are significantly restricting HIV-1 entry and replication in LC
Our results suggest that autophagy flux is dampened upon HIV-1 challenge which might favour virus progression
Summary
Background and aim Our research aims to decipher the mechanism and immune consequences imposed by HIV-mediated modulation of autophagy in challenged dendritic cell (DC) subsets, in particular Langerhans cells (LC). Autophagy is an ubiquitous cellular process involved in lysosomalmediated degradation of host components as well as invading pathogens. HIV-1 was shown to modulate the autophagy flux in various immune cell types, including T cells, macrophages and myeloid dendritic cells. Very little is known about the potential autophagy-driven antiviral activity in LC
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