ORP2 couples LDL‐cholesterol transport to FAK activation by endosomal cholesterol/PI(4,5)P2 exchange

Low‐density lipoprotein (LDL)‐cholesterol delivery from late endosomes to the plasma membrane regulates focal adhesion dynamics and cell migration, but the mechanisms controlling it are poorly characterized. Here, we employed auxin‐inducible rapid degradation of oxysterol‐binding protein‐related pro...

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Bibliographic Details
Published in:The EMBO journal 2021-07, Vol.40 (14), p.e106871-n/a
Main Authors: Takahashi, Kohta, Kanerva, Kristiina, Vanharanta, Lauri, Almeida‐Souza, Leonardo, Lietha, Daniel, Olkkonen, Vesa M, Ikonen, Elina
Format: Article
Language:English
Subjects:
Adhesion
Cell activation
Cell adhesion
Cell migration
Cholesterol
cholesterol trafficking
EMBO20
EMBO21
Endosomes
Exchanging
Focal adhesion kinase
Kinases
Lipid bilayers
Lipids
Low density lipoprotein
Membranes
Npc1 protein
oxysterol‐binding protein‐related protein
phosphoinositides
Plasma
Protein turnover
Proteins
recycling
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Summary:Low‐density lipoprotein (LDL)‐cholesterol delivery from late endosomes to the plasma membrane regulates focal adhesion dynamics and cell migration, but the mechanisms controlling it are poorly characterized. Here, we employed auxin‐inducible rapid degradation of oxysterol‐binding protein‐related protein 2 (ORP2/OSBPL2) to show that endogenous ORP2 mediates the transfer of LDL‐derived cholesterol from late endosomes to focal adhesion kinase (FAK)‐/integrin‐positive recycling endosomes in human cells. In vitro , cholesterol enhances membrane association of FAK to PI(4,5)P 2 ‐containing lipid bilayers. In cells, ORP2 stimulates FAK activation and PI(4,5)P 2 generation in endomembranes, enhancing cell adhesion. Moreover, ORP2 increases PI(4,5)P 2 in NPC1‐containing late endosomes in a FAK‐dependent manner, controlling their tubulovesicular trafficking. Together, these results provide evidence that ORP2 controls FAK activation and LDL‐cholesterol plasma membrane delivery by promoting bidirectional cholesterol/PI(4,5)P 2 exchange between late and recycling endosomes. Synopsis How LDL‐cholesterol is delivered from late endosomes to the plasma membrane and enhances cell motility is unknown. Here, this is found to depend on ORP2‐mediated lipid exchange between late endosomes and focal adhesion kinase (FAK)‐positive recycling endosomes promoting FAK activation. Loss of ORP2 abrogates LDL‐cholesterol delivery from late to recycling endosomes. LDL‐cholesterol activates FAK pending ORP2‐mediated cholesterol transfer. FAK activity promotes PI(4,5)P 2 generation in endosomes, fueling the delivery of LDL‐cholesterol to the plasma membrane. ORP2 controls endomembrane distribution of PI(4,5)P 2 and tubulation of NPC1‐positive endosomes. Graphical Abstract Cholesterol effects on cell motility depend on ORP2‐mediated lipid transfer from late endosomes to focal adhesion kinase‐/integrin‐positive recycling endosomes.
ISSN:0261-4189
1460-2075
DOI:10.15252/embj.2020106871