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A spatiotemporal Notch interaction map from plasma membrane to nucleus

  • Alexandre P. Martin
  • , Gary A. Bradshaw
  • , Robyn J. Eisert
  • , Emily D. Egan
  • , Lena Tveriakhina
  • , Julia M. Rogers
  • , Andrew N. Dates
  • , Gustavo Scanavachi
  • , Jon C. Aster
  • , Tom Kirchhausen
  • , Marian Kalocsay
  • , Stephen C. Blacklow
  • Harvard University
  • Boston Children's Hospital
  • Brigham and Women’s Hospital
  • University of Texas MD Anderson Cancer Center
  • Dana-Farber Cancer Institute

Research output: Contribution to journalArticlepeer-review

17 Scopus citations

Abstract

Notch signaling relies on ligand-induced proteolysis of the transmembrane receptor Notch to liberate a nuclear effector that drives cell fate decisions. Upon ligand binding, sequential cleavage of Notch by the transmembrane protease ADAM10 and the intracellular protease γ-secretase releases the Notch intracellular domain (NICD), which translocates to the nucleus and forms a complex that induces target gene transcription. To map the location and timing of the individual steps required for the proteolysis and movement of Notch from the plasma membrane to the nucleus, we used proximity labeling with quantitative, multiplexed mass spectrometry to monitor the interaction partners of endogenous NOTCH2 after ligand stimulation in the presence of a γ-secretase inhibitor and as a function of time after inhibitor removal. Our studies showed that γ-secretase–mediated cleavage of NOTCH2 occurred in an intracellular compartment and that formation of nuclear complexes and recruitment of chromatin-modifying enzymes occurred within 45 min of inhibitor washout. These findings provide a detailed spatiotemporal map tracking the path of Notch from the plasma membrane to the nucleus and identify signaling events that are potential targets for modulating Notch activity.

Original languageEnglish
Article numbereadg6474
JournalScience Signaling
Volume16
Issue number796
DOIs
StatePublished - Aug 1 2023

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