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Título

Identification of a New Cholesterol-Binding Site within the IFN-γ Receptor that is Required for Signal Transduction

AutorMorana, Ornella CSIC; Nieto-Garai, Jon Ander CSIC ORCID; Björkholm, Patrik; Serna, Jorge Bernardino de la; Terrones, Oihana CSIC ORCID; Arboleya, Aroa CSIC; Ciceri, Dalila CSIC; Rojo-Bartolomé, Iratxe CSIC; Blouin, Cédric M.; Lamaze, Christophe; Lorizate, Maier CSIC ORCID; Contreras, F. Xabier CSIC ORCID
Palabras claveCholesterol
Interferon gamma receptors
Lipid nanodomains
Protein-lipid interactions
Signal transduction
Fecha de publicación14-abr-2022
EditorWiley-VCH
CitaciónAdvanced Science 9(11): 2105170 (2022)
ResumenThe cytokine interferon-gamma (IFN-γ) is a master regulator of innate and adaptive immunity involved in a broad array of human diseases that range from atherosclerosis to cancer. IFN-γ exerts it signaling action by binding to a specific cell surface receptor, the IFN-γ receptor (IFN-γR), whose activation critically depends on its partition into lipid nanodomains. However, little is known about the impact of specific lipids on IFN-γR signal transduction activity. Here, a new conserved cholesterol (chol) binding motif localized within its single transmembrane domain is identified. Through direct binding, chol drives the partition of IFN-γR2 chains into plasma membrane lipid nanodomains, orchestrating IFN-γR oligomerization and transmembrane signaling. Bioinformatics studies show that the signature sequence stands for a conserved chol-binding motif presented in many mammalian membrane proteins. The discovery of chol as the molecular switch governing IFN-γR transmembrane signaling represents a significant advance for understanding the mechanism of lipid selectivity by membrane proteins, but also for figuring out the role of lipids in modulating cell surface receptor function. Finally, this study suggests that inhibition of the chol-IFNγR2 interaction may represent a potential therapeutic strategy for various IFN-γ-dependent diseases.
Versión del editorhttps://doi.org/10.1002/advs.202105170
URIhttp://hdl.handle.net/10261/296403
DOI10.1002/advs.202105170
E-ISSN2198-3844
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