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Aggregability of the SQSTM1/p62-based aggresome-like induced structures determines the sensitivity to parthanatos.

Shuhei HamanoTakuya NoguchiYukino AsaiRyo ItoRyuto KomatsuTetsu SatoAya InoueTomoe MaruyamaTada-Aki KudoYusuke HirataSawako ShindoYasuo UchidaGi-Wook HwangAtsushi Matsuzawa
Published in: Cell death discovery (2024)
Overactivation of poly (ADP-ribose) polymerase-1 (PARP-1) triggers a noncanonical form of programmed cell death (PCD) called parthanatos, yet the mechanisms of its induction are not fully understood. We have recently demonstrated that the aggresome-like induced structures (ALIS) composed of the autophagy receptor SQSTM1/p62 and K48-linked polyubiquitinated proteins (p62-based ALIS) mediate parthanatos. In this study, we identified the D1 dopamine receptor agonist YM435 as a unique parthanatos inhibitor that acts as the disaggregating agent for the p62-based ALIS. We found that YM435 structurally reduces aggregability of the ALIS, and then increases its hydrophilicity and liquidity, which prevents parthanatos. Moreover, dopamine and L-DOPA, a dopamine precursor, also prevented parthanatos by reducing the aggregability of the ALIS. Together, these observations suggest that aggregability of the p62-based ALIS determines the sensitivity to parthanatos, and the pharmacological properties of YM435 that reduces the aggregability may be suitable for therapeutic drugs for parthanatos-related diseases such as neurodegenerative diseases.
Keyphrases
  • high glucose
  • diabetic rats
  • drug induced
  • high resolution
  • oxidative stress
  • signaling pathway
  • cell death
  • mouse model
  • endoplasmic reticulum stress
  • endothelial cells
  • binding protein