Mannose receptor is an HIV restriction factor counteracted by Vpr in macrophages.
Jay LubowMaria C VirgilioMadeline MerlinoDavid R CollinsMichael MashibaBrian G PetersonZana LukicMark M PainterFrancisco Gomez-RiveraValeri H TerryGretchen ZimmermanKathleen L CollinsPublished in: eLife (2020)
HIV-1 Vpr is necessary for maximal HIV infection and spread in macrophages. Evolutionary conservation of Vpr suggests an important yet poorly understood role for macrophages in HIV pathogenesis. Vpr counteracts a previously unknown macrophage-specific restriction factor that targets and reduces the expression of HIV Env. Here, we report that the macrophage mannose receptor (MR), is a restriction factor targeting Env in primary human monocyte-derived macrophages. Vpr acts synergistically with HIV Nef to target distinct stages of the MR biosynthetic pathway and dramatically reduce MR expression. Silencing MR or deleting mannose residues on Env rescues Env expression in HIV-1-infected macrophages lacking Vpr. However, we also show that disrupting interactions between Env and MR reduces initial infection of macrophages by cell-free virus. Together these results reveal a Vpr-Nef-Env axis that hijacks a host mannose-MR response system to facilitate infection while evading MR's normal role, which is to trap and destroy mannose-expressing pathogens.
Keyphrases
- hiv infected
- antiretroviral therapy
- hiv positive
- human immunodeficiency virus
- hiv testing
- hiv aids
- contrast enhanced
- poor prognosis
- magnetic resonance
- hepatitis c virus
- men who have sex with men
- cell free
- endothelial cells
- adipose tissue
- magnetic resonance imaging
- long non coding rna
- gene expression
- dendritic cells
- dna methylation
- cancer therapy
- antimicrobial resistance