Login / Signup

Metastable condensates suppress conversion to amyloid fibrils.

Tapojyoti DasFatima ZaidiMina FaragKiersten M RuffJames MessingJ Paul TaylorRohit V PappuTanja Mittag
Published in: bioRxiv : the preprint server for biology (2024)
Stress granules form via co-condensation of RNA binding proteins with prion-like low complexity domains (PLCDs) and RNA molecules released by stress-induced polysomal runoff. Homotypic interactions among PLCDs can drive amyloid fibril formation and this is enhanced by ALS-associated mutations. We find that homotypic interactions that drive condensation versus fibril formation are separable for A1-LCD, the PLCD of hnRNPA1. These separable interactions lead to condensates that are metastable versus fibrils that are globally stable. Metastable condensates suppress fibril formation, and ALS-associated mutations enhance fibril formation by weakening condensate metastability. Mutations designed to enhance A1-LCD condensate metastability restore wild-type behaviors of stress granules in cells even when ALS-associated mutations are present. This suggests that fibril formation can be suppressed by enhancing condensate metastability through condensate-driving interactions.
Keyphrases
  • stress induced
  • wild type
  • amyotrophic lateral sclerosis
  • induced apoptosis
  • oxidative stress
  • cell cycle arrest
  • heat stress
  • cell death