Mechanisms of regulation and diversification of deubiquitylating enzyme function

Leznicki, Pawel; Kulathu, Yogesh

doi:10.1242/jcs.201855

Cited by 83 publications

(89 citation statements)

References 118 publications

(130 reference statements)

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“…Deubiquitinating enzymes are proteases that cleave ubiquitin off the substrate protein or within ubiquitin moieties in a polyubiquitin chain [91]. The human genome encodes approximately 100 deubiquitinating enzymes, the majority of which are cysteine proteases.…”

Section: The Ubiquitin Systemmentioning

confidence: 99%

Regulation of gap junction intercellular communication by connexin ubiquitination: physiological and pathophysiological implications

Totland

Rasmussen

Knudsen

et al. 2019

Cell. Mol. Life Sci.

102

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Gap junctions consist of arrays of intercellular channels that enable adjacent cells to communicate both electrically and metabolically. Gap junctions have a wide diversity of physiological functions, playing critical roles in both excitable and non-excitable tissues. Gap junction channels are formed by integral membrane proteins called connexins. Inherited or acquired alterations in connexins are associated with numerous diseases, including heart failure, neuropathologies, deafness, skin disorders, cataracts and cancer. Gap junctions are highly dynamic structures and by modulating the turnover rate of connexins, cells can rapidly alter the number of gap junction channels at the plasma membrane in response to extracellular or intracellular cues. Increasing evidence suggests that ubiquitination has important roles in the regulation of endoplasmic reticulum-associated degradation of connexins as well as in the modulation of gap junction endocytosis and post-endocytic sorting of connexins to lysosomes. In recent years, researchers have also started to provide insights into the physiological roles of connexin ubiquitination in specific tissue types. This review provides an overview of the advances made in understanding the roles of connexin ubiquitination in the regulation of gap junction intercellular communication and discusses the emerging physiological and pathophysiological implications of these processes.

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Section: The Ubiquitin Systemmentioning

confidence: 99%

Regulation of gap junction intercellular communication by connexin ubiquitination: physiological and pathophysiological implications

Totland

Rasmussen

Knudsen

et al. 2019

Cell. Mol. Life Sci.

102

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“…Deubiquitinating enzymes (DUBs) exert a variety of important cellular functions, including the control over protein stabilization or degradation, protein localization, protein activity or by modulating protein-protein interactions [50]. We therefore questioned whether inhibition of the deubiquitinase USP7 might affect PRC1.1 stability and function.…”

Section: Usp7 Inhibition Results In Disassembly Of the Prc11 Complexmentioning

confidence: 99%

USP7 as part of non-canonical PRC1.1 is a druggable target in leukemia

Maat

Jaques

López

et al. 2017

Preprint

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Acute myeloid leukemia (AML) is a highly heterogeneous disease in which genetic and epigenetic changes disturb regulatory mechanisms controlling stem cell fate and maintenance. AML still remains difficult to treat, in particular in poor risk AML patients carrying TP53 mutations. Here, we identify the deubiquitinase USP7 as an integral member of non-canonical PRC1.1 and show that targeting of USP7 provides an alternative therapeutic approach for AML. USP7 inhibitors effectively induced apoptosis in (primary) AML cells, also independent of the USP7-MDM2-TP53 axis, whereby survival of both the cycling as well as quiescent populations was affected. MLL-AF9-induced leukemia was significantly delayed in vivo in human leukemia xenografts. We previously showed that non-canonical PRC1.1 is critically important for leukemic stem cell self-renewal, and that genetic knockdown of the PRC1.1 chromatin binding component KDM2B abrogated leukemia development in vitro and in vivo [1]. Here, by performing KDM2B interactome studies in TP53mut cells we identify that USP7 is an essential component of PRC1.1 and is required for its stability and function. USP7 inhibition results in disassembly of the PRC1.1 complex and consequently loss of binding to its target loci. Loss of PRC1.1 binding coincided with reduced H2AK119ub and H3K27ac levels and diminished gene transcription, whereas H3K4me3 levels remained unaffected. Our studies highlight the diverse functions of USP7 and link it to Polycomb-mediated epigenetic control. USP7 inhibition provides an efficient therapeutic approach for AML, also in the most aggressive subtypes with mutations in TP53.Key pointsUSP7 is a therapeutic target in leukemia, including poor risk TP53mut AML.USP7 is an essential component of non-canonical PRC1.1 and is required for its stability and function.

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“…Ubiquitylation is a reversible process, and removal of Ub is carried out by deubiquitylating (DUB) enzymes (eraser module). DUB actions allow the cell to produce monomeric Ub, recycle Ub from chains and reverse signalling events resulting from ubiquitylation [6,7] . To date, 99 DUBs have been identified in the human genome, comprising six major structural families, namely (1) the ubiquitin-specific proteases (USPs), (2) the ubiquitin C-terminal hydrolyses (UCHs), (3) the Machado-Joseph domain proteases (Josephins), (4) the ovarian tumour proteases (OTUs), (5) the Jab1/MPN/Mov34 metalloproteases (JAMM/MPNs) and (6) the newly discovered MIU-containing novel DUB family proteases (MINDYs) (Fig.…”

Section: Introductionmentioning

confidence: 99%

Pseudo-DUBs as allosteric activators and molecular scaffolds of protein complexes

Walden

Masandi

Pawłowski

et al. 2018

Biochemical Society Transactions

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The ubiquitin (Ub) proteasome system and Ub signalling networks are crucial to cell biology and disease development. Deubiquitylases (DUBs) control cell signalling by removing mono-Ub and polyubiquitin chains from substrates. DUBs take part in almost all processes that regulate cellular life and are frequently dysregulated in disease. We have catalogued 99 currently known DUBs in the human genome and sequence conservation analyses of catalytic residues suggest that 11 lack enzyme activity and are classed as pseudo-DUBs. These pseudoenzymes play important biological roles by allosterically activating catalytically competent DUBs as well as other active enzymes. Additionally, pseudoenzymes act as assembly scaffolds of macromolecular complexes. We discuss how pseudo-DUBs have lost their catalytic activity, their diverse mechanisms of action and their potential as therapeutic targets. Many known pseudo-DUBs play crucial roles in cell biology and it is likely that unstudied and overlooked pseudo-DUB genes will have equally important functions.

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Mechanisms of regulation and diversification of deubiquitylating enzyme function

Cited by 83 publications

References 118 publications

Regulation of gap junction intercellular communication by connexin ubiquitination: physiological and pathophysiological implications

Regulation of gap junction intercellular communication by connexin ubiquitination: physiological and pathophysiological implications

USP7 as part of non-canonical PRC1.1 is a druggable target in leukemia

Pseudo-DUBs as allosteric activators and molecular scaffolds of protein complexes

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