Cell Death and Disease (Feb 2021)

Targeted de-repression of neuronal Nrf2 inhibits α-synuclein accumulation

  • Paul S. Baxter,
  • Nóra M. Márkus,
  • Owen Dando,
  • Xin He,
  • Bashayer R. Al-Mubarak,
  • Jing Qiu,
  • Giles E. Hardingham

DOI
https://doi.org/10.1038/s41419-021-03507-z
Journal volume & issue
Vol. 12, no. 2
pp. 1 – 15

Abstract

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Abstract Many neurodegenerative diseases are associated with neuronal misfolded protein accumulation, indicating a need for proteostasis-promoting strategies. Here we show that de-repressing the transcription factor Nrf2, epigenetically shut-off in early neuronal development, can prevent protein aggregate accumulation. Using a paradigm of α-synuclein accumulation and clearance, we find that the classical electrophilic Nrf2 activator tBHQ promotes endogenous Nrf2-dependent α-synuclein clearance in astrocytes, but not cortical neurons, which mount no Nrf2-dependent transcriptional response. Moreover, due to neuronal Nrf2 shut-off and consequent weak antioxidant defences, electrophilic tBHQ actually induces oxidative neurotoxicity, via Nrf2-independent Jun induction. However, we find that epigenetic de-repression of neuronal Nrf2 enables them to respond to Nrf2 activators to drive α-synuclein clearance. Moreover, activation of neuronal Nrf2 expression using gRNA-targeted dCas9-based transcriptional activation complexes is sufficient to trigger Nrf2-dependent α-synuclein clearance. Thus, targeting reversal of the developmental shut-off of Nrf2 in forebrain neurons may alter neurodegenerative disease trajectory by boosting proteostasis.