USP7 Protein (HAUSP Deubiquitinase)

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USP7 Protein (HAUSP Deubiquitinase)

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USP7 Protein (HAUSP Deubiquitinase)

Introduction

USP7 (Ubiquitin-Specific Peptidase 7, also HAUSP; encoded by the [USP7 gene](/genes/usp7)) is a major deubiquitinating enzyme (DUB) that removes ubiquitin from target proteins, rescuing them from proteasomal degradation. USP7 is a critical regulator of the p53/MDM2 axis, epigenetic maintenance, and neuronal proteostasis.

Overview

USP7 is a 128 kDa cysteine protease belonging to the ubiquitin-specific protease (USP) family of deubiquitinating enzymes[1]. It removes ubiquitin moieties from over 70 known substrates, with functional consequences ranging from protein stabilization to altered signaling. USP7's role in balancing the [ubiquitin-proteasome system](/mechanisms/ubiquitin-proteasome-system) makes it relevant to neurodegenerative protein aggregation disorders. [@faesen2011]

<div class="infobox infobox-protein"> [@kategaya2017]

| | | [@hao2015]
|---|---| [@bhatt2020]
| Protein Name | USP7 (HAUSP) | [@turnbull2017]
| Gene | [USP7](/genes/usp7) |
| UniProt ID | [Q93009](https://www.uniprot.org/uniprot/Q93009) |
| Molecular Weight | 128 kDa |
| Length | 1,102 amino acids |
| Subcellular Localization | Nucleus (nuclear bodies), cytoplasm |
| Enzymatic Activity | Cysteine protease; deubiquitinating enzyme |

</div>

Structure

Domain Architecture

USP7 has a modular five-domain architecture[1]:

...

USP7 Protein (HAUSP Deubiquitinase)

Introduction

USP7 (Ubiquitin-Specific Peptidase 7, also HAUSP; encoded by the [USP7 gene](/genes/usp7)) is a major deubiquitinating enzyme (DUB) that removes ubiquitin from target proteins, rescuing them from proteasomal degradation. USP7 is a critical regulator of the p53/MDM2 axis, epigenetic maintenance, and neuronal proteostasis.

Overview

USP7 is a 128 kDa cysteine protease belonging to the ubiquitin-specific protease (USP) family of deubiquitinating enzymes[1]. It removes ubiquitin moieties from over 70 known substrates, with functional consequences ranging from protein stabilization to altered signaling. USP7's role in balancing the [ubiquitin-proteasome system](/mechanisms/ubiquitin-proteasome-system) makes it relevant to neurodegenerative protein aggregation disorders. [@faesen2011]

<div class="infobox infobox-protein"> [@kategaya2017]

| | | [@hao2015]
|---|---| [@bhatt2020]
| Protein Name | USP7 (HAUSP) | [@turnbull2017]
| Gene | [USP7](/genes/usp7) |
| UniProt ID | [Q93009](https://www.uniprot.org/uniprot/Q93009) |
| Molecular Weight | 128 kDa |
| Length | 1,102 amino acids |
| Subcellular Localization | Nucleus (nuclear bodies), cytoplasm |
| Enzymatic Activity | Cysteine protease; deubiquitinating enzyme |

</div>

Structure

Domain Architecture

USP7 has a modular five-domain architecture[1]:

TRAF-like domain (N-terminal, aa 53-205): MATH domain that mediates interactions with p53, MDM2, and many substrates via a P/AxxS motif
Catalytic domain (aa 208-560): USP fold containing the Cys223-His464-Asp481 catalytic triad; cleaves isopeptide bonds between ubiquitin and substrates
Five UBL domains (C-terminal, aa 560-1084): Five tandem ubiquitin-like (UBL) folds that serve as scaffolds for allosteric activation and protein interactions

Catalytic Mechanism

USP7's catalytic domain adopts an auto-inhibited conformation in isolation[2]:

Apo state: The catalytic triad is misaligned; Cys223 is displaced from His464

Ubiquitin binding: Ubiquitin binding induces conformational change, realigning the catalytic triad

Allosteric activation: C-terminal UBL domains (especially UBL4-5 + GMP synthetase) further stabilize the active conformation

Isopeptide hydrolysis: Cys223 attacks the isopeptide bond between ubiquitin's C-terminus and substrate lysine

This auto-inhibition provides a safeguard against uncontrolled deubiquitination.

Function

Substrate Recognition and Regulation

USP7 recognizes substrates primarily through its TRAF-like domain[3]:

| Substrate | Pathway | Consequence of Deubiquitination |
|-----------|---------|--------------------------------|
| p53 | Tumor suppression | Stabilization → cell cycle arrest/apoptosis |
| MDM2 | p53 regulation | Stabilization → increased p53 degradation |
| [DNMT1](/genes/dnmt1) | [DNA methylation](/entities/dna-methylation) | Maintains DNA methylation patterns |
| UHRF1 | Epigenetic maintenance | Chromatin remodeling |
| FOXP3 | Treg function | Stabilizes master Treg transcription factor |
| PTEN | PI3K/Akt signaling | Nuclear PTEN stabilization |
| BMI1/RING1B | Polycomb silencing | Maintains H2A ubiquitination |
| β-catenin | Wnt signaling | Promotes Wnt target gene expression |

Neuronal Roles

In the nervous system, USP7 serves essential functions[4]:

Endosomal recycling: USP7 regulates WASH complex for endosomal protein recycling; loss impairs synaptic receptor trafficking
Epigenetic maintenance: Stabilizes DNMT1 and Polycomb proteins critical for neuronal identity gene programs
Synaptic homeostasis: Modulates turnover of postsynaptic density scaffolding proteins
Neural development: Required for neural crest specification and brain patterning

Role in Neurodegeneration

Tau Deubiquitination

USP7 has been identified as a [tau](/proteins/tau) deubiquitinase with implications for [AD](/diseases/alzheimers-disease)[5]:

USP7 removes ubiquitin from [tau](/proteins/tau), protecting it from proteasomal degradation
In tauopathies, excessive USP7 activity could contribute to tau accumulation
Selective inhibition of USP7's tau-deubiquitinating activity is a potential therapeutic strategy
USP7 is found in neurofibrillary tangle-bearing [neurons](/entities/neurons)

Proteostasis Network

USP7 operates in balance with the ubiquitination machinery[3]:

Opposes [UBA1](/genes/uba1)-initiated ubiquitin cascade by removing ubiquitin from substrates
Dysregulation in either direction disrupts proteostasis:
Too much USP7 → substrates escape degradation → aggregation
Too little USP7 → excessive degradation → Hao-Fountain syndrome

Protein Interactions

| Interactor | Binding Site | Function |
|-----------|-------------|----------|
| Ubiquitin | Catalytic domain | Substrate for cleavage |
| p53 | TRAF domain (P/AxxS) | Tumor suppressor stabilization |
| MDM2 | TRAF domain | E3 ligase stabilization |
| GMP synthetase (GMPS) | UBL4-5 | Allosteric activator |
| DNMT1 | TRAF domain | DNA methyltransferase stabilization |
| WASH complex | TRAF domain | Endosomal recycling regulation |
| ICP0 (HSV) | TRAF domain | Viral immune evasion |

Clinical Significance

USP7 Inhibitors

Multiple USP7-selective inhibitors have been developed for oncology[6]:

GNE-6776: Allosteric inhibitor; blocks ubiquitin binding
FT671/FT827: Active-site inhibitors with high selectivity
P5091: Early-generation compound; less selective
Caution: Neurodevelopmental phenotype of USP7 LoF suggests CNS side effects

Therapeutic Considerations for Neurodegeneration

Partial inhibition: Titrated USP7 inhibition could enhance tau clearance without causing NDD
Substrate-selective modulation: Disrupting USP7-tau interaction while preserving other functions
Combination with proteasome activators: Reduce deubiquitination of tau while enhancing proteasomal clearance

External Links

[USP7 - UniProt](https://www.uniprot.org/uniprot/Q93009)
[USP7 - PDB](https://www.rcsb.org/structure/1NB8)
[USP7 - NCBI Gene](https://www.ncbi.nlm.nih.gov/gene/7874)

References

[Hu M et al., Crystal structure of a UBP-family deubiquitinating enzyme in isolation and in complex with ubiquitin aldehyde (2002) (2002)](https://doi.org/10.1016/S0092-8674(02)

[Faesen AC et al., Mechanism of USP7/HAUSP activation by its C-terminal ubiquitin-like domain and allosteric regulation by GMP-synthetase (2011) (2011)](https://doi.org/10.1016/j.molcel.2011.06.034)

[Kategaya L et al., USP7 small-molecule inhibitors interfere with ubiquitin binding (2017) (2017)](https://doi.org/10.1038/nature24006)

[Hao YH et al., USP7 acts as a molecular rheostat to promote WASH-dependent endosomal protein recycling and is mutated in a human neurodevelopmental disorder (2015) (2015)](https://doi.org/10.1016/j.molcel.2015.09.033)

[Bhatt DG et al., USP7 as a deubiquitinase for tau: implications for Alzheimer's disease (2020) (2020)](https://doi.org/10.1038/s41467-020-17120-x)

[Turnbull AP et al., Molecular basis of USP7 inhibition by selective small-molecule inhibitors (2017) (2017)](https://doi.org/10.1038/nature24451)

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USP7PROTEIN

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📊 Evidence Profile Foundational

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50%

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Outgoing

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📗 Cite This Artifact

USP7 Protein (HAUSP Deubiquitinase)

USP7 Protein (HAUSP Deubiquitinase)

Introduction

Overview

Structure

Domain Architecture

USP7 Protein (HAUSP Deubiquitinase)

Introduction

Overview

Structure

Domain Architecture

Catalytic Mechanism

Function

Substrate Recognition and Regulation

Neuronal Roles

Role in Neurodegeneration

Tau Deubiquitination

Proteostasis Network

Protein Interactions

Clinical Significance

USP7 Inhibitors

Therapeutic Considerations for Neurodegeneration

See Also

External Links

References

💬 Discussion