Interferon-inducible phospholipids govern IFITM3-dependent endosomal antiviral immunity.
Giulia UnaliGiovanni CrivicichIsabel PaganiMonah Abou-AlezzFilippo FolchiniErika ValeriVittoria MataforaJulie A ReiszAnna Maria Sole GiordanoIvan CuccovilloGiacomo M ButtaLorena DonniciAngelo D'AlessandroRaffaele de FrancescoLara ManganaroDavide CittaroIvan MerelliCarolina PetrilloAngela BachiElisa VicenziAnna Kajaste-RudnitskiPublished in: The EMBO journal (2023)
The interferon-induced transmembrane proteins (IFITM) are implicated in several biological processes, including antiviral defense, but their modes of action remain debated. Here, taking advantage of pseudotyped viral entry assays and replicating viruses, we uncover the requirement of host co-factors for endosomal antiviral inhibition through high-throughput proteomics and lipidomics in cellular models of IFITM restriction. Unlike plasma membrane (PM)-localized IFITM restriction that targets infectious SARS-CoV2 and other PM-fusing viral envelopes, inhibition of endosomal viral entry depends on lysines within the conserved IFITM intracellular loop. These residues recruit Phosphatidylinositol 3,4,5-trisphosphate (PIP3) that we show here to be required for endosomal IFITM activity. We identify PIP3 as an interferon-inducible phospholipid that acts as a rheostat for endosomal antiviral immunity. PIP3 levels correlated with the potency of endosomal IFITM restriction and exogenous PIP3 enhanced inhibition of endocytic viruses, including the recent SARS-CoV2 Omicron variant. Together, our results identify PIP3 as a critical regulator of endosomal IFITM restriction linking it to the Pi3K/Akt/mTORC pathway and elucidate cell-compartment-specific antiviral mechanisms with potential relevance for the development of broadly acting antiviral strategies.
Keyphrases
- sars cov
- high throughput
- particulate matter
- transcription factor
- respiratory syndrome coronavirus
- dendritic cells
- air pollution
- single cell
- heavy metals
- mass spectrometry
- oxidative stress
- immune response
- fatty acid
- risk assessment
- mesenchymal stem cells
- drug induced
- endothelial cells
- cell therapy
- water soluble
- diabetic rats