ASO targeting RBM3 temperature‐controlled poison exon splicing prevents neurodegeneration in vivo

Author:

Preußner Marco1ORCID,Smith Heather L23,Hughes Daniel2ORCID,Zhang Min1,Emmerichs Ann‐Kathrin1,Scalzitti Silvia1,Peretti Diego2,Swinden Dean23,Neumann Alexander14,Haltenhof Tom14,Mallucci Giovanna R23ORCID,Heyd Florian1ORCID

Affiliation:

1. Institut für Chemie und Biochemie, RNA Biochemie Freie Universität Berlin Berlin Germany

2. UK Dementia Research Institute and Department of Clinical Neurosciences University of Cambridge Cambridge UK

3. Altos Labs Cambridge Institute of Science Cambridge UK

4. Omiqa Bioinformatics Berlin Germany

Abstract

AbstractNeurodegenerative diseases are increasingly prevalent in the aging population, yet no disease‐modifying treatments are currently available. Increasing the expression of the cold‐shock protein RBM3 through therapeutic hypothermia is remarkably neuroprotective. However, systemic cooling poses a health risk, strongly limiting its clinical application. Selective upregulation of RBM3 at normothermia thus holds immense therapeutic potential. Here we identify a poison exon within the RBM3 gene that is solely responsible for its cold‐induced expression. Genetic removal or antisense oligonucleotide (ASO)‐mediated manipulation of this exon yields high RBM3 levels independent of cooling. Notably, a single administration of ASO to exclude the poison exon, using FDA‐approved chemistry, results in long‐lasting increased RBM3 expression in mouse brains. In prion‐diseased mice, this treatment leads to remarkable neuroprotection, with prevention of neuronal loss and spongiosis despite high levels of disease‐associated prion protein. Our promising results in mice support the possibility that RBM3‐inducing ASOs might also deliver neuroprotection in humans in conditions ranging from acute brain injury to Alzheimer's disease.

Funder

Freie Universität Berlin

UK Dementia Research Institute

Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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