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Intracellular delivery of Parkin-RING0-based fragments corrects Parkin-induced mitochondrial dysfunction through interaction with SLP-2.

Alessandra ZanonMarianna GuidaAlexandros A LavdasCorrado CortiMaria Paulina Castelo RuedaAlessandro NegroPeter P PramstallerFrancisco S DominguesAndrew A HicksIrene Pichler
Published in: Journal of translational medicine (2024)
These findings place further emphasis on the importance of the protein-protein interaction between Parkin and SLP-2 for the maintenance of optimal mitochondrial function. The possibility of restoring an abolished binding to SLP-2 by delivering the Parkin RING0 domain or the Parkin mini-peptide involved in this specific protein-protein interaction into cells might represent a novel organelle-specific therapeutic approach for correcting mitochondrial dysfunction in Parkin-linked PD.
Keyphrases
  • protein protein
  • small molecule
  • cell proliferation
  • endothelial cells