Stimulation of synaptic activity promotes TFEB-mediated clearance of pathological MAPT/Tau in cellular and mouse models of tauopathies.
Yvette AkwaChiara Di MaltaFátima ZalloElise GondardAdele LunatiLara Z Diaz-de-GrenuAngela ZampelliAnne BoiretSara SantamariaMaialen Martinez-PreciadoKatia CorteseJeffrey H KordowerCarlos MatuteAndres M LozanoEstibaliz Capetillo-ZarateThomas VaccariCarmine SettembreEtienne Emile BaulieuDavide TampelliniPublished in: Autophagy (2022)
Synapses represent an important target of Alzheimer disease (AD), and alterations of their excitability are among the earliest changes associated with AD development. Synaptic activation has been shown to be protective in models of AD, and deep brain stimulation (DBS), a surgical strategy that modulates neuronal activity to treat neurological and psychiatric disorders, produced positive effects in AD patients. However, the molecular mechanisms underlying the protective role(s) of brain stimulation are still elusive. We have previously demonstrated that induction of synaptic activity exerts protection in mouse models of AD and frontotemporal dementia (FTD) by enhancing the macroautophagy/autophagy flux and lysosomal degradation of pathological MAPT/Tau. We now provide evidence that TFEB (transcription factor EB), a master regulator of lysosomal biogenesis and autophagy, is a key mediator of this cellular response. In cultured primary neurons from FTD-transgenic mice, synaptic stimulation inhibits MTORC1 signaling, thus promoting nuclear translocation of TFEB, which, in turn, induces clearance of MAPT/Tau oligomers. Conversely, synaptic activation fails to promote clearance of toxic MAPT/Tau in neurons expressing constitutively active RRAG GTPases, which sequester TFEB in the cytosol, or upon TFEB depletion. Activation of TFEB is also confirmed in vivo in DBS-stimulated AD mice. We also demonstrate that DBS reduces pathological MAPT/Tau and promotes neuroprotection in Parkinson disease patients with tauopathy. Altogether our findings indicate that stimulation of synaptic activity promotes TFEB-mediated clearance of pathological MAPT/Tau. This mechanism, underlying the protective effect of DBS, provides encouraging support for the use of synaptic stimulation as a therapeutic treatment against tauopathies.
Keyphrases
- deep brain stimulation
- parkinson disease
- cerebrospinal fluid
- prefrontal cortex
- obsessive compulsive disorder
- transcription factor
- mouse model
- cell death
- signaling pathway
- end stage renal disease
- spinal cord
- oxidative stress
- cerebral ischemia
- endoplasmic reticulum stress
- type diabetes
- endothelial cells
- chronic kidney disease
- newly diagnosed
- spinal cord injury
- blood brain barrier
- adipose tissue
- prognostic factors
- single molecule
- resting state
- wild type
- living cells
- transcranial direct current stimulation
- replacement therapy