Neuronal surface P antigen (NSPA) modulates postsynaptic NMDAR stability through ubiquitination of tyrosine phosphatase PTPMEG.

Sofía EspinozaSebastián B ArredondoFrancisca BarakeFrancisco CarvajalFernanda G GuerreroFabian Segovia-MirandaDavid M ValenzuelaUrsula WynekenAlejandro Rojas-FernándezWaldo CerpaLoreto MassardoLorena Varela-NallarAlfonso González

Published in: BMC biology (2020)

NSPA contributes to hippocampal plasticity and memory processes ensuring appropriate levels of adult neurogenesis and PSD-located NMDAR. PTPMEG qualifies as NSPA ubiquitination substrate that regulates Tyr phosphorylation-dependent NMDAR stability at PSDs. The NSPA/PTPMEG pathway emerges as a new regulator of glutamatergic transmission and plasticity and may provide mechanistic clues and therapeutic opportunities for anti-P-mediated pathogenicity in SLE, a still unmet need.

Keyphrases

cerebral ischemia
systemic lupus erythematosus
protein kinase
working memory
subarachnoid hemorrhage
transcription factor
disease activity
blood brain barrier
rheumatoid arthritis
brain injury
staphylococcus aureus
pseudomonas aeruginosa
young adults
temporal lobe epilepsy
childhood cancer
candida albicans