Journal
NEURON
Volume 96, Issue 2, Pages 355-+Publisher
CELL PRESS
DOI: 10.1016/j.neuron.2017.09.041
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Funding
- ADRC pilot grant (ADRC)
- Competitive Medical Research grant [UPMC-CMRF2013]
- Whitehall Foundation [2013-05-70]
- R21 grant [MH107966]
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Compelling evidence links amyloid beta (Ab) peptide accumulation in the brains of Alzheimer's disease (AD) patients with the emergence of learning and memory deficits, yet a clear understanding of the events that drive this synaptic pathology are lacking. We present evidence that neurons exposed to Ab are unable to form new synapses, resulting in learning deficits in vivo. We demonstrate the Nogo receptor family (NgR1-3) acts as Ab receptors mediating an inhibition of synapse assembly, plasticity, and learning. Live imaging studies reveal Ab activates NgRs on the dendritic shaft of neurons, triggering an inhibition of calcium signaling. We define T-type calcium channels as a target of Ab-NgR signaling, mediating Ab's inhibitory effects on calcium, synapse assembly, plasticity, and learning. These studies highlight deficits in new synapse assembly as a potential initiator of cognitive pathology in AD, and pinpoint calcium dysregulation mediated by NgRs and T-type channels as key components.
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