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Publication : Microglial MERTK eliminates phosphatidylserine-displaying inhibitory post-synapses.

First Author  Park J Year  2021
Journal  EMBO J Volume  40
Issue  15 Pages  e107121
PubMed ID  34013588 Mgi Jnum  J:314434
Mgi Id  MGI:6729770 Doi  10.15252/embj.2020107121
Citation  Park J, et al. (2021) Microglial MERTK eliminates phosphatidylserine-displaying inhibitory post-synapses. EMBO J 40(15):e107121
abstractText  Glia contribute to synapse elimination through phagocytosis in the central nervous system. Despite the important roles of this process in development and neurological disorders, the identity and regulation of the "eat-me" signal that initiates glia-mediated phagocytosis of synapses has remained incompletely understood. Here, we generated conditional knockout mice with neuronal-specific deletion of the flippase chaperone Cdc50a, to induce stable exposure of phosphatidylserine, a well-known "eat-me" signal for apoptotic cells, on the neuronal outer membrane. Surprisingly, acute Cdc50a deletion in mature neurons causes preferential phosphatidylserine exposure in neuronal somas and specific loss of inhibitory post-synapses without effects on other synapses, resulting in abnormal excitability and seizures. Ablation of microglia or the deletion of microglial phagocytic receptor Mertk prevents the loss of inhibitory post-synapses and the seizure phenotype, indicating that microglial phagocytosis is responsible for inhibitory post-synapse elimination. Moreover, we found that phosphatidylserine is used for microglia-mediated pruning of inhibitory post-synapses in normal brains, suggesting that phosphatidylserine serves as a general "eat-me" signal for inhibitory post-synapse elimination.
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