Structural insights into the lysophospholipid brain uptake mechanism and its inhibition by syncytin-2.
Maria Martinez-MolledoEmmanuel NjiNicolas ReyesPublished in: Nature structural & molecular biology (2022)
Brain development and function require uptake of essential omega-3 fatty acids in the form of lysophosphatidylcholine via major-facilitator superfamily transporter MFSD2A, a potential pharmaceutical target to modulate blood-brain barrier (BBB) permeability. MFSD2A is also the receptor of endogenous retroviral envelope syncytin-2 (SYNC2) in human placenta, where it mediates cell-cell fusion and formation of the maternal-fetal interface. Here, we report a cryo-electron microscopy structure of the human MFSD2A-SYNC2 complex that reveals a large hydrophobic cavity in the transporter C-terminal domain to occlude long aliphatic chains. The transporter architecture suggests an alternating-access transport mechanism for lipid substrates in mammalian MFS transporters. SYNC2 establishes an extensive binding interface with MFSD2A, and a SYNC2-soluble fragment acts as a long-sought-after inhibitor of MFSD2A transport. Our work uncovers molecular mechanisms important to brain and placenta development and function, and SYNC2-mediated inhibition of MFSD2A transport suggests strategies to aid delivery of therapeutic macromolecules across the BBB.
Keyphrases
- blood brain barrier
- cerebral ischemia
- endothelial cells
- electron microscopy
- resting state
- fatty acid
- white matter
- single cell
- cell therapy
- functional connectivity
- induced pluripotent stem cells
- pluripotent stem cells
- high resolution
- multiple sclerosis
- physical activity
- brain injury
- binding protein
- body mass index
- weight loss