4.8 Article

Phospholipid-flippase chaperone CDC50A is required for synapse maintenance by regulating phosphatidylserine exposure

EMBO JOURNAL (2021)

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Journal

EMBO JOURNAL
Volume 40, Issue 21, Pages -

Publisher

WILEY
DOI: 10.15252/embj.2021107915

Keywords

CDC50A; GPR56; microglia; phosphatidylserine; synapse elimination

Categories

Biochemistry & Molecular Biology Cell Biology

Funding

  1. NINDS [R01 NS094164, R21 NS108312, P01 NS083513, R01 NS108446]

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Phosphatidylserine exposure at synapses is regulated by CDC50A to protect synapses from erroneous pruning.
Synaptic refinement is a critical physiological process that removes excess synapses to establish and maintain functional neuronal circuits. Recent studies have shown that focal exposure of phosphatidylserine (PS) on synapses acts as an eat me signal to mediate synaptic pruning. However, the molecular mechanism underlying PS externalization at synapses remains elusive. Here, we find that murine CDC50A, a chaperone of phospholipid flippases, localizes to synapses, and that its expression depends on neuronal activity. Cdc50a knockdown leads to phosphatidylserine exposure at synapses and subsequent erroneous synapse removal by microglia partly via the GPR56 pathway. Taken together, our data support that CDC50A safeguards synapse maintenance by regulating focal phosphatidylserine exposure at synapses.

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