| First Author | Martinez TP | Year | 2024 |
| Journal | eNeuro | Volume | 11 |
| Issue | 3 | PubMed ID | 38331575 |
| Mgi Jnum | J:358313 | Mgi Id | MGI:7613528 |
| Doi | 10.1523/ENEURO.0175-23.2024 | Citation | Martinez TP, et al. (2024) Amyloid-beta-induced dendritic spine elimination requires Ca(2+)-permeable AMPA receptors, AKAP-Calcineurin-NFAT signaling, and the NFAT target gene Mdm2. eNeuro 11(3):ENEURO.0175-23.2024 |
| abstractText | Alzheimer's Disease (AD) is associated with brain accumulation of synaptotoxic amyloid-beta (Abeta) peptides produced by the proteolytic processing of amyloid precursor protein (APP). Cognitive impairments associated with AD correlate with dendritic spine and excitatory synapse loss, particularly within the hippocampus. In rodents, soluble Abeta oligomers impair hippocampus-dependent learning and memory, promote dendritic spine loss, inhibit NMDA-type glutamate receptor (NMDAR)-dependent long-term potentiation (LTP), and promote synaptic depression (LTD), at least in part through activation of the Ca(2+)-CaM-dependent phosphatase calcineurin (CaN). Yet, questions remain regarding Abeta-dependent postsynaptic CaN signaling specifically at the synapse to mediate its synaptotoxicity. Here, we use pharmacologic and genetic approaches to demonstrate a role for postsynaptic signaling via A kinase-anchoring protein 150 (AKAP150)-scaffolded CaN in mediating Abeta-induced dendritic spine loss in hippocampal neurons from rats and mice of both sexes. In particular, we found that Ca(2+)-permeable AMPA-type glutamate receptors (CP-AMPARs), which were previously shown to signal through AKAP-anchored CaN to promote both LTD and Abeta-dependent inhibition of LTP, are also required upstream of AKAP-CaN signaling to mediate spine loss via overexpression of APP containing multiple mutations linked to familial, early-onset AD and increased Abeta production. In addition, we found that the CaN-dependent nuclear factor of activated T-cells (NFAT) transcription factors are required downstream to promote Abeta-mediated dendritic spine loss. Finally, we identified the E3-ubiquitin ligase Mdm2, which was previously linked to LTD and developmental synapse elimination, as a downstream NFAT target gene upregulated by Abeta whose enzymatic activity is required for Abeta-mediated spine loss.Significance Statement Impaired hippocampal function and synapse loss are hallmarks of AD linked to Abeta oligomers. Abeta exposure acutely blocks hippocampal LTP and enhances LTD and chronically leads to dendritic spine synapse loss. In particular, Abeta hijacks normal plasticity mechanisms, biasing them toward synapse weakening/elimination, with previous studies broadly linking CaN phosphatase signaling to this synaptic dysfunction. However, we do not understand how Abeta engages signaling specifically at synapses. Here we elucidate a synapse-to-nucleus signaling pathway coordinated by the postsynaptic scaffold protein AKAP150 that is activated by Ca(2+) influx through CP-AMPARs and transduced to nucleus by CaN-NFAT signaling to transcriptionally upregulate the E3-ubiquitin ligase Mdm2 that is required for Abeta-mediated spine loss. These findings identify Mdm2 as potential therapeutic target for AD. |
