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Activity-dependent tau cleavage by caspase-3 promotes neuronal dysfunction and synaptotoxicity

Carli K. Opland, Miles R. Bryan, Braxton Harris, Jake McGillion-Moore, Xu Tian, Youjun Chen, Michelle S. Itano, Graham H. Diering, Rick B. Meeker, Todd J. Cohen

2023iScience17 citationsDOIOpen Access PDF

Abstract

Tau-mediated toxicity is associated with cognitive decline and Alzheimer's disease (AD) progression. In particular, tau post-translational modifications (PTMs) are thought to generate aberrant tau species resulting in neuronal dysfunction. Despite being well characterized in postmortem AD brain, it is unclear how caspase-mediated C-terminal tau cleavage promotes neurodegeneration, as few studies have developed the models to dissect this pathogenic mechanism. Here, we show that proteasome impairment results in cleaved tau accumulation at the post-synaptic density (PSD), a process that is modulated by neuronal activity. Cleaved tau (at residue D421) impairs neuronal firing and causes inefficient initiation of network bursts, consistent with reduced excitatory drive. We propose that reduced neuronal activity, or silencing, is coupled to proteasome dysfunction, which drives cleaved tau accumulation at the PSD and subsequent synaptotoxicity. Our study connects three common themes in the progression of AD: impaired proteostasis, caspase-mediated tau cleavage, and synapse degeneration.

Topics & Concepts

Cleavage (geology)NeuroscienceChemistryCell biologyCaspase 3CaspaseBiophysicsApoptosisBiologyBiochemistryProgrammed cell deathFracture (geology)PaleontologyNeuroscience and Neuropharmacology ResearchAlzheimer's disease research and treatmentsComputational Drug Discovery Methods
Activity-dependent tau cleavage by caspase-3 promotes neuronal dysfunction and synaptotoxicity | Litcius