Nuclear ERK1/2 signaling potentiation enhances neuroprotection and cognition via Importinα1/KPNA2.
Marzia IndrigoIlaria MorellaDaniel OrellanaRaffaele d' IsaAlessandro PapaleRiccardo ParraAntonia GurgoneDaniela LeccaAnna CavacciniCezar M TigaretAlfredo CagnottoKimberley JonesSimon BrooksGian Michele RattoNicholas D AllenMariah J LelosSilvia MiddeiMaurizio GiustettoAnna R CartaRaffaella ToniniMario SalmonaJeremy HallKerrie ThomasRiccardo BrambillaStefania FasanoPublished in: EMBO molecular medicine (2023)
Cell signaling is central to neuronal activity and its dysregulation may lead to neurodegeneration and cognitive decline. Here, we show that selective genetic potentiation of neuronal ERK signaling prevents cell death in vitro and in vivo in the mouse brain, while attenuation of ERK signaling does the opposite. This neuroprotective effect mediated by an enhanced nuclear ERK activity can also be induced by the novel cell penetrating peptide RB5. In vitro administration of RB5 disrupts the preferential interaction of ERK1 MAP kinase with importinα1/KPNA2 over ERK2, facilitates ERK1/2 nuclear translocation, and enhances global ERK activity. Importantly, RB5 treatment in vivo promotes neuroprotection in mouse models of Huntington's (HD), Alzheimer's (AD), and Parkinson's (PD) disease, and enhances ERK signaling in a human cellular model of HD. Additionally, RB5-mediated potentiation of ERK nuclear signaling facilitates synaptic plasticity, enhances cognition in healthy rodents, and rescues cognitive impairments in AD and HD models. The reported molecular mechanism shared across multiple neurodegenerative disorders reveals a potential new therapeutic target approach based on the modulation of KPNA2-ERK1/2 interactions.