Nature Communications (Sep 2023)

Altered ubiquitin signaling induces Alzheimer’s disease-like hallmarks in a three-dimensional human neural cell culture model

  • Inbal Maniv,
  • Mahasen Sarji,
  • Anwar Bdarneh,
  • Alona Feldman,
  • Roi Ankawa,
  • Elle Koren,
  • Inbar Magid-Gold,
  • Noa Reis,
  • Despina Soteriou,
  • Shiran Salomon-Zimri,
  • Tali Lavy,
  • Ellina Kesselman,
  • Naama Koifman,
  • Thimo Kurz,
  • Oded Kleifeld,
  • Daniel Michaelson,
  • Fred W. van Leeuwen,
  • Bert M. Verheijen,
  • Yaron Fuchs,
  • Michael H. Glickman

DOI
https://doi.org/10.1038/s41467-023-41545-7
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 14

Abstract

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Abstract Alzheimer’s disease (AD) is characterized by toxic protein accumulation in the brain. Ubiquitination is essential for protein clearance in cells, making altered ubiquitin signaling crucial in AD development. A defective variant, ubiquitin B + 1 (UBB+1), created by a non-hereditary RNA frameshift mutation, is found in all AD patient brains post-mortem. We now detect UBB+1 in human brains during early AD stages. Our study employs a 3D neural culture platform derived from human neural progenitors, demonstrating that UBB+1 alone induces extracellular amyloid-β (Aβ) deposits and insoluble hyperphosphorylated tau aggregates. UBB+1 competes with ubiquitin for binding to the deubiquitinating enzyme UCHL1, leading to elevated levels of amyloid precursor protein (APP), secreted Aβ peptides, and Aβ build-up. Crucially, silencing UBB+1 expression impedes the emergence of AD hallmarks in this model system. Our findings highlight the significance of ubiquitin signalling as a variable contributing to AD pathology and present a nonclinical platform for testing potential therapeutics.