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RBM3 mediates structural plasticity and protective effects of cooling in neurodegeneration

descriptionPublicationkeyboard_double_arrow_right Article , Other literature type 14 Jan 2015Embargo end date: 09 Nov 2017 United Kingdom English Publisher:Springer Science and Business Media LLCJournal:Nature, volume 518, pages 236-239 (issn: 0028-0836, eissn: 1476-4687, Copyright policy )Funded by:UKRI | Multi-donor allogeneic hu...
Authors: Peretti, D; Bastide, A; Radford, H; Verity, N; Molloy, C; Martin, MG; Moreno, JA; +5 Authors

doi: 10.1038/nature14142 , 10.17863/cam.14501

pmid: 25607368

pmc: PMC4338605

handle: 2381/43389

RBM3 mediates structural plasticity and protective effects of cooling in neurodegeneration

Abstract

In the healthy adult brain synapses are continuously remodelled through a process of elimination and formation known as structural plasticity. Reduction in synapse number is a consistent early feature of neurodegenerative diseases, suggesting deficient compensatory mechanisms. Although much is known about toxic processes leading to synaptic dysfunction and loss in these disorders, how synaptic regeneration is affected is unknown. In hibernating mammals, cooling induces loss of synaptic contacts, which are reformed on rewarming, a form of structural plasticity. We have found that similar changes occur in artificially cooled laboratory rodents. Cooling and hibernation also induce a number of cold-shock proteins in the brain, including the RNA binding protein, RBM3 (ref. 6). The relationship of such proteins to structural plasticity is unknown. Here we show that synapse regeneration is impaired in mouse models of neurodegenerative disease, in association with the failure to induce RBM3. In both prion-infected and 5XFAD (Alzheimer-type) mice, the capacity to regenerate synapses after cooling declined in parallel with the loss of induction of RBM3. Enhanced expression of RBM3 in the hippocampus prevented this deficit and restored the capacity for synapse reassembly after cooling. RBM3 overexpression, achieved either by boosting endogenous levels through hypothermia before the loss of the RBM3 response or by lentiviral delivery, resulted in sustained synaptic protection in 5XFAD mice and throughout the course of prion disease, preventing behavioural deficits and neuronal loss and significantly prolonging survival. In contrast, knockdown of RBM3 exacerbated synapse loss in both models and accelerated disease and prevented the neuroprotective effects of cooling. Thus, deficient synapse regeneration, mediated at least in part by failure of the RBM3 stress response, contributes to synapse loss throughout the course of neurodegenerative disease. The data support enhancing cold-shock pathways as potential protective therapies in neurodegenerative disorders.

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United Kingdom
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Keywords

Male, 571, Neuronal Plasticity, Animal, Prions, Cold-Shock Response, RNA-Binding Proteins, Neurodegenerative Diseases, Hippocampus, Article, Cold Temperature, Disease Models, Animal, Mice, Neuroprotective Agents, Alzheimer Disease, Hibernation, Disease Models, Synapses, Cold Shock Proteins and Peptides, Animals, Regeneration

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citations
This is an alternative to the "Influence" indicator, which also reflects the overall/total impact of an article in the research community at large, based on the underlying citation network (diachronically).
BIP!Citations provided by BIP!
popularity
This indicator reflects the "current" impact/attention (the "hype") of an article in the research community at large, based on the underlying citation network.
BIP!Popularity provided by BIP!
influence
This indicator reflects the overall/total impact of an article in the research community at large, based on the underlying citation network (diachronically).
BIP!Influence provided by BIP!
impulse
This indicator reflects the initial momentum of an article directly after its publication, based on the underlying citation network.
BIP!Impulse provided by BIP!
212
Top 1%
Top 1%
Top 1%
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