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USP7 protects TFEB from proteasome-mediated degradation

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Peer-reviewed

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https://www.repository.cam.ac.uk/handle/1810/374279

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Primary Published version (4.45 MB)

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Article

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Authors

Rubinsztein, David  ORCID logo  https://orcid.org/0000-0001-5002-5263

Abstract

The transcription factor EB (TFEB) is a master regulator of lysosomal biogenesis and autophagy. We identify a distinct nuclear interactome of TFEB, with USP7 emerging as a key post-translational modulator of TFEB. Genetic depletion and inhibition of USP7 reveal its critical role in preserving TFEB stability within both nuclear and cytoplasmic compartments. Specifically, USP7 is identified as the deubiquitinase responsible for removing the K48-linked polyubiquitination signal from TFEB at lysine residues K116, K264, and K274, thereby preventing its proteasomal degradation. Functional assays demonstrate the involvement of USP7 in preserving TFEB-mediated transcriptional responses to nutrient deprivation, while also modulating autophagy flux and lysosome biogenesis. As USP7 is a deubiquitinase that protects TFEB from proteasomal degradation, these findings provide the foundation for therapeutic targeting of the USP7-TFEB axis in conditions characterized by TFEB dysregulation and metabolic abnormalities, particularly in certain cancers.

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Keywords

CP: Cell biology, CP: Molecular biology, TFEB, USP7, autophagy, lysosomal biogenesis, post-translational modifications, proteasomal degradation, ubiquitination, Ubiquitin-Specific Peptidase 7, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Humans, Proteasome Endopeptidase Complex, Autophagy, Ubiquitination, Proteolysis, HEK293 Cells, Lysosomes, Animals, HeLa Cells, Cell Nucleus

Journal Title

Cell Reports

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Journal ISSN

2211-1247
2211-1247

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Publisher

Elsevier

Publisher DOI

https://doi.org/10.1016/j.celrep.2024.114872

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Attribution 4.0 International
Except where otherwised noted, this item's license is described as Attribution 4.0 International
Sponsorship
UK Dementia Research Institute (Unknown)
National Institute for Health and Care Research (IS-BRC-1215-20014)
We are grateful for funding from the UK Dementia Research Institute principally funded by the Medical Research Council, and the NIHR Cambridge Biomedical Research Centre (BRC-1215-20014). SK is funded by the Cambridge Commonwealth, European & International Trust, the Nehru Trust for Cambridge University, and the Trinity-Henry Barlow Scholarship. MT is funded by the Rosetrees Trust and the Cambridge University School of Clinical Medicine (James Baird Fund and F.E. Elmore Fund).

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Is supplemented by:
https://doi.org/• The mass spectrometry proteomics data have been deposited to the ProteomeXchange Consortium via the PRIDE partner repository with the dataset identifier PXD055937.

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University of Cambridge Research Outputs (Articles and Conferences)