USP13: Multiple Functions and Target Inhibition

Li, Xiaolong; Yang, Ge; Zhang, Wenyao; Qin, Biying; Ye, Zifan; Shi, Huijing; Zhao, Xinmeng; Chen, Yihang; Song, Bowei; Mei, Ziqing; Zhao, Qi; Wang, Feng

doi:10.3389/fcell.2022.875124

Cited by 9 publications

(6 citation statements)

References 104 publications

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“…24,27,41 USP13 is a deubiquitinase that modulates cancer progression, immune inflammatory response, metabolism disorder. 28 Several studies have shown that USP13 exerted important functions in modulating lung fibrosis and ECM deposition. Knockdown of USP13 accelerated lung fibroblasts phenotypic changes and contributed to pulmonary fibrosis.…”

Section: Discussionmentioning

confidence: 99%

“…Ubiquitin-specific protease 13 (USP13) is a vital factor in innate immune responses, energy metabolism, autophagy, DNA damage response in different diseases, and can act as a tumor promoter in cancers. 28 Reports have found that USP13 was critical in the pathogenetic mechanism of pulmonary fibrosis, and knockdown of USP13 promoted lung fibroblasts phenotypic changes and contributes to pulmonary fibrosis. 29,30 Besides, USP13 overexpression reversed the repression of Spautin-1-induced autophagy and ferroptosis in cerebral ischemia-reperfusion injury.…”

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confidence: 99%

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LncRNA FRMD6‐AS1/miR‐491‐5p/USP13 pathway attenuated ferroptosis and contributed to liver fibrosis

Li,

Zou,

Jin

et al. 2024

Environmental Toxicology

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Liver fibrosis is an invertible pathophysiologic process featured by excessive accumulation of extracellular matrix (ECM) which injures liver cells and activates hepatic stellate cells (HSCs). Besides, inducing ferroptosis in activated HSCs can alleviate liver fibrosis. LncRNAs modulate ferroptosis in activated HSCs and ECM deposition in liver fibrosis. However, the role of lncRNA FRMD6‐AS1 in liver fibrosis is not discovered. In this study, lncRNA FRMD6‐AS1 was dramatically up‐regulated in activated HSCs. Knockdown of FRMD6‐AS1 markedly increased iron ion, ROS and MDA levels, decreased GSH level, SLC7A11 and GPX4 protein expressions in activated HSCs. In addition, HSCs activation markers α‐SMA and COL1α1 expressions were up‐regulated in activated HSCs; knockdown of FRMD6‐AS1 markedly down‐regulated α‐SMA and COL1α1 expressions in HSCs. Besides, lncRNA FRMD6‐AS1 could interact with miR‐491‐5p, and negatively modulate miR‐491‐5p expression. USP13 was a target of miR‐491‐5p, and could be negatively modulated by miR‐491‐5p. Moreover, FRMD6‐AS1 knockdown increased iron ion and ROS levels, decreased SLC7A11 and GPX4 protein expressions, facilitated HSCs viability, and up‐regulated α‐SMA and COL1α1 expressions via miR‐491‐5p/USP13 pathway. Finally, FRMD6‐AS1 knockdown restored liver tissue structure and abrogated fibrosis in livers in a CCL4 liver fibrosis mouse model. Hence, lncRNA FRMD6‐AS1/miR‐491‐5p/USP13 pathway repressed ferroptosis, promoted ECM deposition and facilitated liver fibrosis in vitro and in vivo models.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

LncRNA FRMD6‐AS1/miR‐491‐5p/USP13 pathway attenuated ferroptosis and contributed to liver fibrosis

Li,

Zou,

Jin

et al. 2024

Environmental Toxicology

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Section: Deubiquitinating Enzymes (Dubs) That Regulate Parkin Functionmentioning

confidence: 99%

“…Ataxin 3 has been reported to directly interact with Parkin and regulates its ubiquitylation [ 72 , 73 , 75 ]. Ataxin 3 has a preference for K63-linked Ub chains and plays an important role in DNA repair and endoplasmatic reticulum-associated degradation [ 72 ]. The catalytic activity of Ataxin 3 is regulated via its N-terminal Josephin domain, whereas the C-terminal domain containing the Ub-interacting motif controls which interacts with different substates including Parkin [ 72 , 75 ].…”

Section: Deubiquitinating Enzymes (Dubs) That Regulate Parkin Functionmentioning

confidence: 99%

“…Ataxin 3 has a preference for K63-linked Ub chains and plays an important role in DNA repair and endoplasmatic reticulum-associated degradation [ 72 ]. The catalytic activity of Ataxin 3 is regulated via its N-terminal Josephin domain, whereas the C-terminal domain containing the Ub-interacting motif controls which interacts with different substates including Parkin [ 72 , 75 ]. Mutations in Ataxin 3 have been associated with Machado-Joseph disease where Parkin degradation was accelerated via the autophagy pathway [ 73 , 75 ].…”

Section: Deubiquitinating Enzymes (Dubs) That Regulate Parkin Functionmentioning

confidence: 99%

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Targeting Deubiquitinating Enzymes (DUBs) That Regulate Mitophagy via Direct or Indirect Interaction with Parkin

Tsefou

Ketteler

2022

IJMS

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The quality control of mitochondria is critical for the survival of cells, and defects in the pathways required for this quality control can lead to severe disease. A key quality control mechanism in cells is mitophagy, which functions to remove damaged mitochondria under conditions of various stresses. Defective mitophagy can lead to a number of diseases including neurodegeneration. It has been proposed that an enhancement of mitophagy can improve cell survival, enhance neuronal function in neurodegeneration and extend health and lifespans. In this review, we highlight the role of deubiquitinating enzymes (DUBs) in the regulation of mitophagy. We summarise the current knowledge on DUBs that regulate mitophagy as drug targets and provide a list of small molecule inhibitors that are valuable tools for the further development of therapeutic strategies targeting the mitophagy pathway in neurodegeneration.

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Identification of Ubiquitination-Associated Proteins Using 2D-DIGE

Dowling

Bazou

2022

Methods in Molecular Biology

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USP13: Multiple Functions and Target Inhibition

Cited by 9 publications

References 104 publications

LncRNA FRMD6‐AS1/miR‐491‐5p/USP13 pathway attenuated ferroptosis and contributed to liver fibrosis

LncRNA FRMD6‐AS1/miR‐491‐5p/USP13 pathway attenuated ferroptosis and contributed to liver fibrosis

Targeting Deubiquitinating Enzymes (DUBs) That Regulate Mitophagy via Direct or Indirect Interaction with Parkin

Identification of Ubiquitination-Associated Proteins Using 2D-DIGE

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