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638 results on '"Ubiquitin binding"'

1. A novel RNF125 variant associated with Tenorio syndrome alters ubiquitin chain binding.

Author

Barzak, Fareeda M., Lu, Anita, Geltzeiler, Alexa R., Ledgerwood, Elizabeth C., Chung, Wendy K., and Day, Catherine L.

Abstract

A key signalling pathway required for clearance of viruses from host cells relies on the receptor protein, retinoic acid‐inducible gene I (RIG‐I). The activity of RIG‐I is tightly controlled, and once bound to viral dsRNA, addition of lysine 63‐linked ubiquitin chains activates signalling. Meanwhile, the addition of lysine 48‐linked ubiquitin chains to RIG‐I is required to terminate signalling when the infection has been resolved. Really interesting new gene (RING) finger protein 125 (RNF125) is the E3 ligase responsible for addition of the ubiquitin chains that terminate signalling, with disruption of its function associated with Tenorio syndrome. Here we describe a novel RNF125 gene variant in an individual with clinical symptoms including intellectual disability, macrocephaly and congenital heart disease, consistent with Tenorio syndrome. The newly identified Tenorio syndrome‐associated variant [(NM_017831.4):c.670G>C p.Glu224Gln] is the first to be found in the ubiquitin interaction motif (UIM) of RNF125. While the E3 ligase activity of this RNF125 variant is retained, it has an impaired ability to interact with lysine 63‐linked ubiquitin chains. The function of the UIM in RNF125 is uncertain; however, this study suggests that the UIM binds lysine 63‐linked ubiquitin chains, and that this interaction is required for the normal function of RNF125. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Structure–Activity Relationship of USP5 Inhibitors

Author

Rachel Harding, M.K. Mann, Ahmed Aman, Carlos Zepeda-Velázquez, Brian J. Wilson, Taira Kiyota, Cheryl H. Arrowsmith, Peter Loppnau, Rima Al-awar, Matthieu Schapira, Héctor González-Álvarez, Yanjun Li, and Aiping Dong

Subjects
Ubiquitin binding, Cleavage (embryo), Deubiquitinating enzyme, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Endopeptidases, Drug Discovery, Humans, Structure–activity relationship, Enzyme Inhibitors, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Dose-Response Relationship, Drug, Molecular Structure, biology, Chemistry, Substrate (chemistry), In vitro, 3. Good health, Enzyme, Biochemistry, biology.protein, Molecular Medicine, 030217 neurology & neurosurgery, Function (biology)
Abstract

USP5 is a deubiquitinase that has been implicated in a range of diseases, including cancer, but no USP5-targeting chemical probe has been reported to date. Here, we present the progression of a chemical series that occupies the C-terminal ubiquitin-binding site of a poorly characterized zinc-finger ubiquitin binding domain (ZnF-UBD) of USP5 and competitively inhibits the catalytic activity of the enzyme. Exploration of the structure-activity relationship, complemented with crystallographic characterization of the ZnF-UBD bound to multiple ligands, led to the identification of 64, which binds to the USP5 ZnF-UBD with a KD of 2.8 μM and is selective over nine proteins containing structurally similar ZnF-UBD domains. 64 inhibits the USP5 catalytic cleavage of a di-ubiquitin substrate in an in vitro assay. This study provides a chemical and structural framework for the discovery of a chemical probe to delineate USP5 function in cells.

Published
2021

4. Cryo-EM structure of human Pol κ bound to DNA and mono-ubiquitylated PCNA

Author

Vlad-Stefan Raducanu, Alfredo De Biasio, Souvika Bakshi, Ramon Crehuet, Masateru Takahashi, Matthew Percival, Samir M. Hamdan, Timothy J. Ragan, Frederick W. Muskett, Mohamed Abdelmaboud Sobhy, Muhammad Tehseen, Claudia Lancey, Kerry Blair, and Ministerio de Economía y Competitividad (España)

Subjects
Ubiquitin binding, DNA polymerase, DNA damage, viruses, Science, General Physics and Astronomy, DNA-Directed DNA Polymerase, Protomer, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ubiquitin, Cryoelectron microscopy, Proliferating Cell Nuclear Antigen, Humans, Polymerase, 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, Ubiquitination, General Chemistry, DNA, Proliferating cell nuclear antigen, chemistry, biology.protein, Biophysics, 030217 neurology & neurosurgery, DNA Damage, Protein Binding
Abstract

Y-family DNA polymerase κ (Pol κ) can replicate damaged DNA templates to rescue stalled replication forks. Access of Pol κ to DNA damage sites is facilitated by its interaction with the processivity clamp PCNA and is regulated by PCNA mono-ubiquitylation. Here, we present cryo-EM reconstructions of human Pol κ bound to DNA, an incoming nucleotide, and wild type or mono-ubiquitylated PCNA (Ub-PCNA). In both reconstructions, the internal PIP-box adjacent to the Pol κ Polymerase-Associated Domain (PAD) docks the catalytic core to one PCNA protomer in an angled orientation, bending the DNA exiting the Pol κ active site through PCNA, while Pol κ C-terminal domain containing two Ubiquitin Binding Zinc Fingers (UBZs) is invisible, in agreement with disorder predictions. The ubiquitin moieties are partly flexible and extend radially away from PCNA, with the ubiquitin at the Pol κ-bound protomer appearing more rigid. Activity assays suggest that, when the internal PIP-box interaction is lost, Pol κ is retained on DNA by a secondary interaction between the UBZs and the ubiquitins flexibly conjugated to PCNA. Our data provide a structural basis for the recruitment of a Y-family TLS polymerase to sites of DNA damage., This research was supported by King Abdullah University of Science and Technology through core funding (to S.M.H.) and the Competitive Research Award Grant CRG8 URF/1/4036‐01‐01 (to S.M.H. and A.D.B.), and by the Wellcome Trust (to A.D.B.). R.C. acknowledges funding from the MINECO (CTQ2016-78636-P) and to AGAUR, (2017 SGR 324). The MD project has been carried out using CSUC resources. We acknowledge The Midlands Regional Cryo-EM Facility at the Leicester Institute of Structural and Chemical Biology (LISCB), major funding from MRC (MC_PC_17136). We thank Christos Savva (LISCB, University of Leicester) for his help in cryo-EM data collection and advice on data processing.

Published
2021

5. Posttranslational modification and beyond: interplay between histone deacetylase 6 and heat-shock protein 90

Author

Kaio Kitazato, Xiaowei Song, Ping Liu, Zhe Ren, Wang Yifei, Yiliang Wang, Ji Xiao, and Lianzhou Huang

Subjects
Ubiquitin binding, Hsp90, Drug development, Review, RM1-950, QD415-436, Histone Deacetylase 6, Biochemistry, Histones, Structure-Activity Relationship, Heat shock protein, Drug Discovery, Genetics, Animals, Humans, HSP90 Heat-Shock Proteins, HSF1, Molecular Biology, Genetics (clinical), Client proteins, biology, Chemistry, Acetylation, HDAC6, Cell biology, Isoenzymes, Histone, Gene Expression Regulation, biology.protein, Molecular Medicine, Histone deacetylase, Therapeutics. Pharmacology, Protein Processing, Post-Translational, Protein Binding, Signal Transduction
Abstract

Posttranslational modification (PTM) and regulation of protein stability are crucial to various biological processes. Histone deacetylase 6 (HDAC6), a unique histone deacetylase with two functional catalytic domains (DD1 and DD2) and a ZnF-UBP domain (ubiquitin binding domain, BUZ), regulates a number of biological processes, including gene expression, cell motility, immune response, and the degradation of misfolded proteins. In addition to the deacetylation of histones, other nonhistone proteins have been identified as substrates for HDAC6. Hsp90, a molecular chaperone that is a critical modulator of cell signaling, is one of the lysine deacetylase substrates of HDAC6. Intriguingly, as one of the best-characterized regulators of Hsp90 acetylation, HDAC6 is the client protein of Hsp90. In addition to regulating Hsp90 at the post-translational modification level, HDAC6 also regulates Hsp90 at the gene transcription level. HDAC6 mainly regulates the Hsp90-HSF1 complex through the ZnF-UBP domain, thereby promoting the HSF1 entry into the nucleus and activating gene transcription. The mutual interaction between HDAC6 and Hsp90 plays an important role in the regulation of protein stability, cell migration, apoptosis and other functions. Plenty of of studies have indicated that blocking HDAC6/Hsp90 has a vital regulatory role in multifarious diseases, mainly in cancers. Therefore, developing inhibitors or drugs against HDAC6/Hsp90 becomes a promising development direction. Herein, we review the current knowledge on molecular regulatory mechanisms based on the interaction of HDAC6 and Hsp90 and inhibition of HDAC6 and/or Hsp90 in oncogenesis and progression, antiviral and immune-related diseases and other vital biological processes.

Published
2021

8. Active site alanine mutations convert deubiquitinases into high‐affinity ubiquitin‐binding proteins.

Author

Morrow, Marie E., Morgan, Michael T., Clerici, Marcello, Growkova, Katerina, Yan, Ming, Komander, David, Sixma, Titia K., Simicek, Michal, and Wolberger, Cynthia

Abstract

Abstract: A common strategy for exploring the biological roles of deubiquitinating enzymes (DUBs) in different pathways is to study the effects of replacing the wild‐type DUB with a catalytically inactive mutant in cells. We report here that a commonly studied DUB mutation, in which the catalytic cysteine is replaced with alanine, can dramatically increase the affinity of some DUBs for ubiquitin. Overexpression of these tight‐binding mutants thus has the potential to sequester cellular pools of monoubiquitin and ubiquitin chains. As a result, cells expressing these mutants may display unpredictable dominant negative physiological effects that are not related to loss of DUB activity. The structure of the SAGA DUB module bound to free ubiquitin reveals the structural basis for the 30‐fold higher affinity of Ubp8C146A for ubiquitin. We show that an alternative option, substituting the active site cysteine with arginine, can inactivate DUBs while also decreasing the affinity for ubiquitin. [ABSTRACT FROM AUTHOR]

Published
2018
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9. Catalytic domain mutation in CYLD inactivates its enzyme function by structural perturbation and induces cell migration and proliferation.

Author

Johari, Tanu and Maiti, Tushar Kanti

Subjects
*UBIQUITIN, *CELL cycle, *DNA repair, *CELL migration, *CELL proliferation
Abstract

Tumor suppressor cylindromatosis protein (CYLD), which specifically cleaves lysine 63-linked ubiquitin chain from its substrate molecules, contributes to myriad of important cellular events including cellular differentiation, oncogenesis, DNA repair and cell cycle control. It is a ubiquitously expressed protein, which negatively regulates NF-kB and JNK signaling pathways and mediates caspase dependent apoptosis through RIP1 deubiqutination. Germline mutations in CYLD are associated with a rare, hypertrophic skin cancer, termed Familial Cylindromatosis. Catalogue of Somatic Mutations in Cancer database ensembles accumulating CYLD point mutations in multiple benign and malignant tumors. However, the functional role of CYLD mutations and their association with cancer progression remains elusive. In the present report, we have shown that cancer associated mutations impose structural alteration in CYLD which impairs its binding to K63 ubiquitin chain. Here, we conclude that loss of CYLD catalytic activity potentiates its oncogenic gain of function through increased cell survival and migration. [ABSTRACT FROM AUTHOR]

Published
2018
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10. The F-box E3 ubiquitin ligase BAF1 mediates the degradation of the brassinosteroid-activated transcription factor BES1 through selective autophagy in Arabidopsis

Author

Yanhai Yin, Trevor M. Nolan, Natalie M. Clark, Ping Wang, Diane C. Bassham, Justin W. Walley, Christian Montes-Serey, Hao Jiang, and Hongqing Guo

Subjects
Ubiquitin binding, biology, Arabidopsis Proteins, Ubiquitin-Protein Ligases, Autophagy, Arabidopsis, Membrane Proteins, Nuclear Proteins, Cell Biology, Plant Science, biology.organism_classification, Ubiquitin ligase, Cell biology, DNA-Binding Proteins, chemistry.chemical_compound, chemistry, Ubiquitin, Proteasome, Brassinosteroids, biology.protein, Brassinosteroid, Transcription factor
Abstract

Brassinosteroids (BRs) regulate plant growth, development, and stress responses by activating the core transcription factor BRI1-EMS-SUPPRESSOR1 (BES1), whose degradation occurs through the proteasome and autophagy pathways. The E3 ubiquitin ligase(s) that modify BES1 for autophagy-mediated degradation remain to be fully defined. Here, we identified an F-box family E3 ubiquitin ligase named BES1-ASSOCIATED F-BOX1 (BAF1) in Arabidopsis thaliana. BAF1 interacts with BES1 and mediates its ubiquitination and degradation. Our genetic data demonstrated that BAF1 inhibits BR signaling in a BES1-dependent manner. Moreover, BAF1 targets BES1 for autophagic degradation in a selective manner. BAF1-triggered selective autophagy of BES1 depends on the ubiquitin binding receptor DOMINANT SUPPRESSOR OF KAR2 (DSK2). Sucrose starvation-induced selective autophagy of BES1, but not bulk autophagy, was significantly compromised in baf1 mutant and BAF1-ΔF (BAF1 F-box decoy) overexpression plants, but clearly increased by BAF1 overexpression. The baf1 and BAF1-ΔF overexpression plants had increased BR-regulated growth but were sensitive to long-term sucrose starvation, while BAF1 overexpression plants had decreased BR-regulated growth but were highly tolerant of sucrose starvation. Our results not only established BAF1 as an E3 ubiquitin ligase that targets BES1 for degradation through selective autophagy pathway, but also revealed a mechanism for plants to reduce growth during sucrose starvation.

Published
2021

11. Selective Recognition and Separation of Ubiquitin by Nanoparticle Embedded Cryogel Traps with Ubiquitin Memories Based on Photosensitive Covalent Imprinting

Author

Filiz Yılmaz, İbrahim Dolak, Arzu Ersöz, Rıdvan Say, Rüstem Keçili, Dicle Üniversitesi, Diyarbakır Teknik Bilimler Meslek Yüksekokulu, Kimya ve Kimyasal İşleme Teknolojileri Bölümü, and Dolak, İbrahim

Subjects
chemistry.chemical_classification, Ubiquitin binding, Ubiquitin, Chemistry, Biomolecule, 010401 analytical chemistry, Molecularly imprinted polymer, Nanoparticle, 010402 general chemistry, 01 natural sciences, Combinatorial chemistry, Separation, 0104 chemical sciences, Analytical Chemistry, Recognition, Covalent bond, Ionic strength, Photosensitive covalently imprinted polymers, Drug delivery, Nanoparticles, Biosensor
Abstract

WOS:000620937600003 Recognition and determination of ubiquitin (Ubq) is very important since it affects the enzymatic mechanisms, which causes damages in the living organisms. This can lead to diseases especially in neuronal system. Molecularly imprinted polymers (MIPs) are selective resins that exhibit high affinity toward target compounds. MIPs have attracted significicant research interest because of their various applications in solid phase extraction, biosensors and drug delivery, etc. Various MIP types can be used such as thermo-sensitive, pH-sensitive, biomolecule-sensitive, ion-sensitive and photo-sensitive in these applications. Photosensitive MIPs can be used to increase the selectivity and binding efficiency to decrease denaturation of target biomolecules. The aim of this study is to prepare photosensitive cross-linked p(Ubq-co-MACys-Ru(bipyr)(2)-MACys) polymeric nanoparticles (UbqINPs) and leach with 0.5 M HCl to create Ubq memories onto nanoparticles (UbqINPs) and optimize their binding parameters in cryogel based column system. For this purpose, different factors such as pH, flow rate, ionic strength and temperature were investigated, and maximum ubiquitin binding capacity was found to be 25 mg/g at pH 7. The results showed that the UbqINPs can be considered as a good binding material for recognition and separation of Ubq.

Published
2021

12. Preclinical Evaluation of an 18F-Labeled SW-100 Derivative for PET Imaging of Histone Deacetylase 6 in the Brain

Author

Kenji Ishii, Jun Toyohara, and Tetsuro Tago

Subjects
chemistry.chemical_classification, 0303 health sciences, Hydroxamic acid, medicine.diagnostic_test, Ubiquitin binding, Physiology, Cognitive Neuroscience, Cell Biology, General Medicine, HDAC6, Protein degradation, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Enzyme, Neuroimaging, chemistry, Positron emission tomography, medicine, Radioligand, 030217 neurology & neurosurgery, 030304 developmental biology
Abstract

Histone deacetylase 6 (HDAC6), an enzyme involved in protein degradation, exhibits several unique properties, such as cytoplasmic localization and ubiquitin binding. HDAC6 has emerged as an interesting therapeutic target in the treatment of neurodegenerative disorders such as Alzheimer's and Parkinson's diseases. Techniques enabling noninvasive HDAC6 imaging in the brain could enhance understanding of its pathologic role, but development of brain-penetrating radioligands for HDACs imaging by positron emission tomography (PET) remains challenging. Here, we report the synthesis and evaluation of an 18F-labeled tetrahydroquinoline derivative, [18F]2, based on the HDAC6 selective inhibitor SW-100 as a brain HDAC6 imaging radioligand. [18F]2 was synthesized via copper-mediated radiofluorination from an arylboronic precursor, followed by removal of the catalyst by solid-phase extraction and then hydroxamic acid formation. [18F]2 demonstrated good penetration and moderate stability in the mouse brain. In mouse plasma, however, [18F]2 was rapidly metabolized to a corresponding carboxylic acid form. Blocking studies in mice with unlabeled compound 2 and HDAC6 selective inhibitors, including tubastatin A and ACY-775, demonstrated that the HDAC6 inhibitors displaced over 80% of [18F]2 taken up in the brain, indicating selective binding of [18F]2. These results suggest that [18F]2 is a potentially useful PET radioligand for brain HDAC6 imaging.

Published
2021

13. Chicken optineurin suppresses MDA5-mediated interferon β production

Author

Yaqing Mao, Huansheng Wu, Jing Xiao, Wenbo Zhang, Yu Li, Ning Jiang, and Xiangdong Wu

Subjects
Interferon-Induced Helicase, IFIH1, animal structures, Ubiquitin binding, chicken optineurin, Chicken Cells, Cell Cycle Proteins, Chick Embryo, Infectious bursal disease virus, Infectious bursal disease, Cell Line, 03 medical and health sciences, medicine, Animals, chicken interferon β, 030304 developmental biology, Optineurin, RNA, Double-Stranded, lcsh:SF1-1100, 0303 health sciences, Messenger RNA, Chemistry, 0402 animal and dairy science, RNA, MDA5, 04 agricultural and veterinary sciences, General Medicine, Interferon-beta, Immunology, Health and Disease, medicine.disease, Birnaviridae Infections, chicken MDA5, 040201 dairy & animal science, inhibition, Cell biology, RNA silencing, Gene Expression Regulation, embryonic structures, Animal Science and Zoology, lcsh:Animal culture, Chickens
Abstract

Chicken MDA5 (chMDA5), the essential accepted pattern recognition receptors for detecting cytoplasmic viral RNA in chicken, initiates interferon β (IFN-β) generation. However, there is an incomplete elucidation of regulating chMDA5-mediated IFN-β production. NEMO-related protein, optineurin, was identified as inhibitors of virus triggered IFN-β induction in human or mice. In this study, full length of chicken optineurin (chOPTN) was cloned from chicken embryo fibroblast, and its role in inhibiting IFN-β signaling pathway was further explored. Full-length chOPTN encodes 547 amino acids residues and contains unique LC3 interaction region and ubiquitin binding domain. Chicken optineurin mRNA and protein are widely expressed in different tissues, especially the heart, kidney, and bursal fabricius (BF). Overexpressed chOPTN not only inhibits poly I:C or homos-induced human IFN-β promoter activation in 293T cells but also suppresses poly I:C, infectious bursal disease virus (IBDV) genome double-strand RNA (dsRNA), and chMDA5-induced chicken IFN-β (chIFN-β) promoter activation. In addition, we first revealed that chOPTN negatively regulates chIFN-β production via inhibiting ubiquitination of chicken TBK1, which is dependent on the ubiquitin-binding domain of chOPTN. Moreover, chIFN-β stimulus, poly I:C, and IBDV genome dsRNA improve chOPTN expression. Endogenous chOPTN expression is also upregulated by IBDV infection in 293T, DF-1 cells, as well as in BF. Therefore, our results suggested that chOPTN plays an inhibition role of chMDA5-mediated chIFN-β signaling pathway in chicken cells.

Published
2021

14. Neurodevelopmental disorder caused by a truncating de novo variant of IRF2BPL

Author

Li Cao, Hui-Dong Tang, Guang Chen, Ze-Yu Zhu, Xiaoxuan Song, Xiao-ying Liu, Jingying Wu, Xiao-Hang Qian, and Shi-Ge Wang

Subjects
Ubiquitin binding, Gene mutation, Biology, medicine.disease_cause, Genetic analysis, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Neurodevelopmental disorder, Exome Sequencing, medicine, Humans, Child, Gene, Genetics, Sanger sequencing, Mutation, Nuclear Proteins, Electroencephalography, General Medicine, medicine.disease, Neurology, Neurodevelopmental Disorders, symbols, Female, Neurology (clinical), Carrier Proteins, IRF2, 030217 neurology & neurosurgery
Abstract

Background Mutations in the IRF2BPL gene can cause neurodevelopmental disorders. We describe the clinical and genetic characteristics of a Chinese patient with a novel abnormality in this gene, explore the potential pathogenic mechanism and summarize the clinical characteristics of 25 patients with IRF2BPL mutations. Methods We identified the gene mutation sites by whole-exome and Sanger sequencing. The protein-protein interaction network of the IRF2BPL gene was constructed using bioinformatic techniques, and its function was enriched. We conducted a functional experiment to explore the potential pathogenicity of the identified IRF2BPL gene mutation. Results An 8-year-old girl presented with progressive cerebellar ataxia, including involuntary tremor and slurred speech. Electroencephalography and electromyography revealed no abnormalities. Structural cranial MRI was also normal, but genetic analysis identified a truncating de novo variant in IRF2BPL. Bioinformatics predicted that IRF2BPL would be associated with IRF2 and 10 other genes and involved in ubiquitin binding and other pathways. The cellular location of IRF2BPL was altered, and compared to control cells, the level of ubiquitinated proteins was significantly decreased in cells harbouring the mutation. Conclusion In this study, we identified a truncating de novo variant of IRF2BPL as a causative gene in the neurodevelopmental disorder of a Chinese girl. Impairment of the ubiquitin-proteasome pathway caused by this IRF2BPL mutation may play an important role in this neurodevelopmental disorder.

Published
2021

15. Diagnosing and mitigating method-based avidity artifacts that confound polyubiquitin-binding assays

Author

Elizabeth Helgason, Allyn J. Schoeffler, Nataliya Popovych, and Erin C. Dueber

Subjects
Bridging (networking), Ubiquitin binding, biology, Computer science, Correction, macromolecular substances, Computational biology, environment and public health, Ubiquitin, Posttranslational modification, biology.protein, Avidity, Polyubiquitin binding, Binding affinities
Abstract

Polyubiquitination is a complex form of posttranslational modification responsible for the control of numerous cellular processes. Many ubiquitin-binding proteins recognize distinct polyubiquitin chain types, and these associations help drive ubiquitin-signaling pathways. There is considerable interest in understanding the specificity of ubiquitin-binding proteins; however, because of the multivalent nature of polyubiquitin, affinity measurements of these interactions that rely on affixing ubiquitin-binding proteins to a surface can display artifactual, method-dependent avidity, or "bridging." This artifact, which is distinct from biologically relevant, avid interactions with polyubiquitin, is commonplace in such polyubiquitin-binding measurements and can lead to dramatic overestimations of binding affinities for particular chain types, and thus, incorrect conclusions about specificity. Here, we use surface-based measurements of ubiquitin binding in three model systems to illustrate bridging and lay out practical ways of identifying and mitigating it. Specifically, we describe a simple fitting model that enables researchers to diagnose the severity of bridging artifacts, determine whether they can be minimized, and more accurately evaluate polyubiquitin-binding specificity.

Published
2022

16. HDAC6 ZnF UBP as the Modifier of Tau Structure and Function

Author

Hariharakrishnan Chidambaram, Abha Dangi, Udaya Kiran Marelli, Abhishek Ankur Balmik, and Subashchandrabose Chinnathambi

Subjects
Models, Molecular, Ubiquitin binding, Protein Conformation, Tau protein, Protein domain, tau Proteins, In Vitro Techniques, Molecular Dynamics Simulation, Histone Deacetylase 6, Biochemistry, Protein Aggregates, 03 medical and health sciences, Microscopy, Electron, Transmission, Catalytic Domain, Humans, Protein Interaction Domains and Motifs, Nuclear Magnetic Resonance, Biomolecular, Zinc finger, 0303 health sciences, biology, Protein Stability, Ubiquitin, Chemistry, 030302 biochemistry & molecular biology, Zinc Fingers, HDAC6, Cell biology, Molecular Docking Simulation, Acetylation, Proteolysis, biology.protein, Histone deacetylase, Cortactin, Protein Binding
Abstract

Histone deacetylase 6 is a class II histone deacetylase primarily present in the cytoplasm and involved in the regulation of various cellular functions. It consists of two catalytic deacetylase domains and a unique zinc finger ubiquitin binding protein domain, which sets it apart from other HDACs. HDAC6 is known to regulate cellular activities by modifying the function of microtubules, HSP90, and cortactin through deacetylation. Apart from the catalytic activity of HDAC6, it interacts with other proteins through either the SE14 domain or the ZnF UBP domain to modulate their functions. Here, we have studied the role of the HDAC6 ZnF UBP domain as a modifier of Tau aggregation by its direct interaction with the polyproline region/repeat region of Tau. Interaction of HDAC6 ZnF UBP with Tau was found to reduce the propensity of Tau to self-aggregate and to disaggregate preformed aggregates in a concentration-dependent manner and also bring about the conformational changes in Tau protein. The interaction of HDAC6 ZnF UBP with Tau results in its degradation, suggesting either proteolytic activity of HDAC6 ZnF UBP or its role in enhancing autoproteolysis of Tau.

Published
2020

17. The Two Deubiquitinating Enzymes from Chlamydia trachomatis Have Distinct Ubiquitin Recognition Properties

Author

Jiaqi Fu, Jiazhang Qiu, Aditya Babar, Zhao-Qing Luo, John M Hausman, Sebastian Kenny, Shalini Iyer, and Chittaranjan Das

Subjects
biology, Ubiquitin binding, Chemistry, Protein domain, Plasma protein binding, medicine.disease_cause, Biochemistry, Deubiquitinating enzyme, Ubiquitin, biology.protein, medicine, Binding site, Chlamydia trachomatis, Deubiquitination
Abstract

Chlamydia trachomatis is the cause of several diseases such as sexually transmitted urogenital disease and ocular trachoma. The pathogen contains a small genome yet, upon infection, expresses two enzymes with deubiquitinating activity, termed ChlaDUB1 and ChlaDUB2, presumed to have redundant deubiquitinase (DUB) function because of the similarity of the primary structure of their catalytic domain. Previous studies have led to structural characterization of the enzymatic properties of ChlaDUB1; however, ChlaDUB2 has yet to be investigated thoroughly. In this study, we investigated the deubiquitinase properties of ChlaDUB2 and compared them to those of ChlaDUB1. This revealed a distinct difference in hydrolytic activity with regard to di- and polyubiquitin chains while showing similar ability to cleave a monoubiquitin-based substrate, ubiquitin aminomethylcoumarin (Ub-AMC). ChlaDUB2 was unable to cleave a diubiquitin substrate efficiently, whereas ChlaDUB1 could rapidly hydrolyze this substrate like a prototypical prokaryotic DUB, SdeA. With polyubiquitinated green fluorescent protein substrate (GFP-Ubn), whereas ChlaDUB1 efficiently disassembled the polyubiquitin chains into the monoubiquitin product, the deubiquitination activity of ChlaDUB2, while showing depletion of the substrate, did not produce appreciable levels of the monoubiquitin product. We report the structures of a catalytic construct of ChlaDUB2 and its complex with ubiquitin propargyl amide. These structures revealed differences in residues involved in substrate recognition between the two Chlamydia DUBs. On the basis of the structures, we conclude that the distal ubiquitin binding is equivalent between the two DUBs, consistent with the Ub-AMC activity result. Therefore, the difference in activity with longer ubiquitinated substrates may be due to the differential recognition of these substrates involving additional ubiquitin binding sites.

Published
2020

18. Radiosynthesis and preliminary evaluation of an 18 F-labeled tubastatin A analog for PET imaging of histone deacetylase 6

Author

Jun Toyohara, Kenji Ishii, and Tetsuro Tago

Subjects
Biodistribution, Hydroxamic acid, medicine.diagnostic_test, Ubiquitin binding, 010405 organic chemistry, Organic Chemistry, Radiosynthesis, HDAC6, Ligand (biochemistry), 01 natural sciences, Biochemistry, Molecular biology, HDAC1, 030218 nuclear medicine & medical imaging, 0104 chemical sciences, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Positron emission tomography, Drug Discovery, medicine, Radiology, Nuclear Medicine and imaging, Spectroscopy
Abstract

Histone deacetylase 6 (HDAC6) is a unique member of the HDAC family because of its characteristics, namely, its cytoplasmic localization and ubiquitin binding. HDAC6 has been implicated in cancer metastasis and neurodegeneration. In the present study, we performed radiosynthesis and biological evaluation of a fluorine-18-labeled ligand [18 F]3, which is an analog of the HDAC6-selective inhibitor tubastatin A, for positron emission tomography (PET) imaging. [18 F]3 was synthesized by a two-step reaction composed of 18 F-fluorination and formation of a hydroxamic acid group. IC50 values of 3 against HDAC1 and HDAC6 activities were 996 nM and 33.1 nM, respectively. A biodistribution study in mice demonstrated low brain uptake of [18 F]3. Furthermore, bone radioactivity was stable at around 2% ID/g after injection, suggesting high tolerance to defluorination. Regarding metabolic stability, 70% of the compound was observed as the unchanged form at 30 minutes post injection in mouse plasma. A small animal PET study in mice showed that pretreatment with cyclosporine A had no effect on initial brain uptake of [18 F]3, suggesting low brain uptake of [18 F]3 was not caused by the P-glycoprotein-mediated efflux. While PET imaging using [18 F]3 has a limitation with respect to neurodegenerative diseases, further studies evaluating its utility for certain cancers are worth evaluating.

Published
2020

19. Total chemical synthesis of the phosphorylated p62 UBA domain reveals that Ser407Pi but not Ser403Pi enhances ubiquitin binding

Author

Ling Xu, Yan Zhang, Xian-Fu Lu, and Yi-Ming Li

Subjects
Autophagosome, biology, Ubiquitin binding, Chemistry, Organic Chemistry, Autophagy, Isothermal titration calorimetry, Native chemical ligation, Biochemistry, Chemical synthesis, Cell biology, Ubiquitin, biology.protein, Phosphorylation, Physical and Theoretical Chemistry
Abstract

As an autophagic adaptor, p62 specifically targets ubiquitinated proteins to an autophagosome for lysosomal degradation through a critical ubiquitin-associated (UBA) domain. Recent research studies reported that the Ser403 and Ser407 sites on the UBA domain were modified by phosphorylation, increasing the binding affinity between p62 and ubiquitin (Ub). However, the exact role of each phosphorylation site in the regulation of the UBA domain and Ub binding remains unclear. In this text, we applied total chemical synthesis to prepare four types of phosphorylated UBAs, among which the bisphosphorylated UBA was successfully synthesized via the pseudo-dipeptide unit and auxiliary-mediated hydrazide-based native chemical ligation (NCL). Isothermal titration calorimetry (ITC) assays showed that the phosphorylation at S407 enhanced the binding affinity between UBA and Ub, while that at S403 did not. It was suggested that phosphorylation at S407 might be important for promoting the interplay between the UBA domain and Ub, whereas phosphorylation at S403 was not directly involved in this interaction.

Published
2020

20. The Ubiquitin-Binding Protein OsDSK2a Mediates Seedling Growth and Salt Responses by Regulating Gibberellin Metabolism in Rice

Author

Rongfeng Huang, Yun Zhou, Juan Wang, Hua Qin, Pengcheng Wei, Haiwen Zhang, Shirong Zhou, and Yuchen Miao

Subjects
0106 biological sciences, 0301 basic medicine, Ubiquitin binding, Mutant, Receptors, Cytoplasmic and Nuclear, Plant Science, Salt Stress, 01 natural sciences, 03 medical and health sciences, Plant Growth Regulators, Ubiquitin, Gene Expression Regulation, Plant, Polyubiquitin, Receptor, Plant Proteins, Oryza sativa, biology, food and beverages, Oryza, Cell Biology, Metabolism, Plants, Genetically Modified, biology.organism_classification, Gibberellins, Cell biology, 030104 developmental biology, Seedlings, Seedling, biology.protein, Salts, Gibberellin, Carrier Proteins, Research Article, 010606 plant biology & botany
Abstract

UBL-UBA (ubiquitin-like-ubiquitin-associated) proteins are ubiquitin receptors and transporters in the ubiquitin-proteasome system that play key roles in plant growth and development. High salinity restricts plant growth by disrupting cellular metabolism, but whether UBL-UBA proteins are involved in this process is unclear. Here, we demonstrate that the UBL-UBA protein OsDSK2a (DOMINANT SUPPRESSOR of KAR2) mediates seedling growth and salt responses in rice (Oryza sativa). Through analysis of osdsk2a, a mutant with retarded seedling growth, as well as in vitro and in vivo assays, we demonstrate that OsDSK2a combines with polyubiquitin chains and interacts with the gibberellin (GA)-deactivating enzyme ELONGATED UPPERMOST INTERNODE (EUI), resulting in its degradation through the ubiquitin-proteasome system. Bioactive GA levels were reduced, and plant growth was retarded in the osdsk2a mutant. By contrast, eui mutants displayed increased seedling growth and bioactive GA levels. OsDSK2a levels decreased in plants under salt stress. Moreover, EUI accumulated under salt stress more rapidly in osdsk2a than in wild-type plants. Thus, OsDSK2a and EUI play opposite roles in regulating plant growth under salt stress by affecting GA metabolism. Under salt stress, OsDSK2a levels decrease, thereby increasing EUI accumulation, which promotes GA metabolism and reduces plant growth.

Published
2019

21. Mechanistic insights into the enhancement or inhibition of phase separation by polyubiquitin chains of different lengths or linkages

Author

Thuy P. Dao, Yiran Yang, Maria F. Presti, Michael S. Cosgrove, Jesse B. Hopkins, Weikang Ma, Stewart N. Loh, and Carlos A. Castañeda

Subjects
Crosstalk (biology), Stress granule, Ubiquitin, biology, Ubiquitin binding, Chemistry, Phase (matter), Biophysics, biology.protein, Affinities
Abstract

SummaryUbiquitin-binding shuttle UBQLN2 mediates crosstalk between proteasomal degradation and autophagy, likely via interactions with K48- and K63-linked polyubiquitin chains, respectively. UBQLN2 is recruited to stress granules in cells and undergoes liquid-liquid phase separation (LLPS) in vitro. However, interactions with ubiquitin or multivalent K48-linked chains eliminate LLPS. Here, we found that, although some polyubiquitin chain types (K11-Ub4 and K48-Ub4) did generally inhibit UBQLN2 LLPS, others (K63-Ub4, M1-Ub4 and a designed tetrameric ubiquitin construct) significantly enhanced LLPS. Using nuclear magnetic resonance (NMR) spectroscopy and complementary biophysical techniques, we demonstrated that these opposing effects stem from differences in chain conformations, but not in affinities between chains and UBQLN2. Chains with extended conformations and increased accessibility to the ubiquitin binding surface significantly promoted UBQLN2 LLPS by enabling a switch between homotypically to partially heterotypically-driven phase separation. Our study provides mechanistic insights into how the structural and conformational properties of polyubiquitin chains contribute to heterotypic phase separation with ubiquitin-binding shuttles and adaptors.HighlightsUbiquitin or short polyubiquitin chains bind to phase separation-driving stickers on UBQLN2 and inhibit its phase separation whereas longer chains provide the multivalency needed to enhance UBQLN2 phase separation.Phase separation of UBQLN2 is promoted over a wide range of Ub:UBQLN2 ratios in the presence of extended M1- and K63-linked Ub4 chains, but not compact K11- and K48-linked Ub4 chains.Chain conformation and accessibility of the Ub interacting surface is a driving factor of UBQLN2/polyUb co-phase separation.UBQLN2 condensates assemble during in vitro enzymatic assembly of K63-linked polyUb chains as free ubiquitin is reduced.

Published
2021

22. Substrate-assisted activation and selectivity of the bacterial RavD effector deubiquitinylase

Author

Eric Schulze-Niemand, Matthias Stein, and Michael Naumann

Subjects
chemistry.chemical_classification, Ubiquitin binding, biology, Effector, Chemistry, Ubiquitin, Ubiquitination, Cleavage (embryo), Biochemistry, Protein–protein interaction, Legionella pneumophila, Enzyme, Bacterial Proteins, Structural Biology, Catalytic triad, Biophysics, biology.protein, Humans, Binding site, Molecular Biology, Protein Binding
Abstract

Deubiquitinylases (DUBs) catalyze the peptide bond cleavage of specific ubiquitin linkages at distinct protein substrates. Pathogens from viruses and bacteria independently developed effector proteins with DUB activity to mimic host DUB functions and circumvent immune responses. The effector protein RavD from Legionella pneumophila cleaves linear ubiquitin chains with an exclusive methionine-1 selectivity. It thus performs as a functional analogue of the human DUB OTULIN, which achieves its selectivity only via a specialized proximal ubiquitin S1' binding site as well as a substrate-assisted activation of the catalytic triad. An analysis of the crystal structures of bacterial RavD in its free and di-ubiquitin-bound forms, in order to rationalize the structural basis for its selectivity and activation mechanism, is not fully conclusive. As these ambiguities might arise from the introduced double mutation of the di-ubiquitin substrate in the RavD-di-ubiquitin complex crystal structure, biomolecular modeling, and molecular dynamics sampling (1-2 μs for each system of RavD and OTULIN) were employed to reconstitute the physiological RavD-di-ubiquitin complex. The simulations show that the distal S1 ubiquitin binding sites of RavD and OTULIN are similar in terms of interface area, composition, and ubiquitin binding affinity. The proximal S1' site of RavD, in contrast, is significantly smaller and ubiquitin binding is weaker and more flexible than in OTULIN. Upon substrate access, the residues of the catalytic triad of RavD show a reduction of flexibility and a conformational transition toward a catalytically active state. Thus, the enzymatic activation of RavD is presumably also substrate-assisted and a clear rationale for the common M1-substrate selectivity.

Published
2021

23. N4BP1 is dimerization-dependent linear ubiquitin reader regulating TNFR1 signalling through linear ubiquitin binding and Caspase-8-mediated processing

Author

Arianna Fornili, James A. Garnett, Irene Pinzuti, Simone Kunzelmann, David Kuntin, Benjamin Stieglitz, Simone Schaubeck, Koraljka Husnjak, Katarzyna Kliza, Kay Hofmann, Wei Song, and Alessandro Pandini

Subjects
Programmed cell death, biology, Ubiquitin binding, Chemistry, Caspase 8, Proinflammatory cytokine, law.invention, Cell biology, Ubiquitin, Proteasome, Apoptosis, law, biology.protein, Suppressor
Abstract

Signalling through TNFR1 modulates proinflammatory gene transcription and programmed cell death, and its impairment causes autoimmune diseases and cancer. NEDD4-binding protein 1 (N4BP1) was recently identified as a critical suppressor of proinflammatory cytokine production1, whose mode of action remained unknown. Here, we show that N4BP1 is a novel linear ubiquitin reader that negatively regulates NFκB signalling by its unique dimerizationdependent ubiquitin-binding module that we named LUBIN. Dimeric N4BP1 strategically positions two non-selective ubiquitin-binding domains to ensure exclusive recognition of linear ubiquitin. Under proinflammatory conditions, N4BP1 is recruited to the nascent TNFR1 signalling complex, where it regulates duration of proinflammatory signalling in LUBIN-dependent manner. N4BP1 deficiency accelerates TNFα-induced cell death by increasing complex II assembly. Under proapoptotic conditions, Caspase-8 mediates proteolytic processing of N4BP1 and the resulting cleavage fragment of N4BP1, which retains the ability to bind linear ubiquitin, is rapidly degraded by the 26S proteasome, accelerating apoptosis. In summary, our findings demonstrate that N4BP1 dimerization creates a unique linear ubiquitin reader that ensures timely and coordinated regulation of TNFR1-mediated inflammation and cell death.

Published
2021

25. TNK1 is a ubiquitin-binding and 14-3-3-regulated kinase that can be targeted to block tumor growth

Author

Christina M. Egbert, Jeffrey W. Tyner, Gaelle Mercenne, Jonard Corpuz Valdoz, Logan Larsen, Tsz-Yin Chan, James D. Moody, Julia E. Maxson, Kristina Kohler, Tsz-Ming Tsang, Kenneth A. Christensen, Madison Frey, Courtney J. Banks, David J. Bearss, Adam Siddiqui, Tetyana V. Forostyan, Joshua L. Andersen, Huimin Geng, Jason M. Foulks, Savannah Free, Erik J. Soderblom, Thomas O'Hare, Steven L. Warner, David C.S. Huang, Katie L. Pennington, Eranga Roshan Balasooriya, Markus Müschen, and Clifford J. Whatcott

Subjects
Fetal Proteins, Ubiquitin binding, bcr-abl, Fusion Proteins, bcr-abl, General Physics and Astronomy, Mice, Ubiquitin, STAT5 Transcription Factor, 2.1 Biological and endogenous factors, Lymphocytes, Aetiology, Cancer, Tumor, Multidisciplinary, biology, Kinase, Chemistry, Protein-Tyrosine Kinases, Tumor Burden, Cell biology, Gene Expression Regulation, Neoplastic, Phosphorylation, Tyrosine kinase, Signal Transduction, Protein Binding, STAT3 Transcription Factor, Cell signaling, Science, Antineoplastic Agents, General Biochemistry, Genetics and Molecular Biology, Cell Line, In vivo, Cell Line, Tumor, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Animals, Humans, Kinase activity, Protein Kinase Inhibitors, Neoplastic, Phospholipase C gamma, Fusion Proteins, General Chemistry, Survival Analysis, Xenograft Model Antitumor Assays, Pyrimidines, HEK293 Cells, 14-3-3 Proteins, Gene Expression Regulation, A549 Cells, biology.protein
Abstract

TNK1 is a non-receptor tyrosine kinase with poorly understood biological function and regulation. Here, we identify TNK1 dependencies in primary human cancers. We also discover a MARK-mediated phosphorylation on TNK1 at S502 that promotes an interaction between TNK1 and 14-3-3, which sequesters TNK1 and inhibits its kinase activity. Conversely, the release of TNK1 from 14-3-3 allows TNK1 to cluster in ubiquitin-rich puncta and become active. Active TNK1 induces growth factor-independent proliferation of lymphoid cells in cell culture and mouse models. One unusual feature of TNK1 is a ubiquitin-association domain (UBA) on its C-terminus. Here, we characterize the TNK1 UBA, which has high affinity for poly-ubiquitin. Point mutations that disrupt ubiquitin binding inhibit TNK1 activity. These data suggest a mechanism in which TNK1 toggles between 14-3-3-bound (inactive) and ubiquitin-bound (active) states. Finally, we identify a TNK1 inhibitor, TP-5801, which shows nanomolar potency against TNK1-transformed cells and suppresses tumor growth in vivo. The mechanisms underlying the activity of non-receptor tyrosine kinase, TNK1, in cancers are unclear. Here the authors show that MARK mediates 14-3-3 and TNK1 interaction which restrains TNK1 activity, while the release of TNK1 from 14-3-3 leads to TNK1 activation through its interaction with ubiquitin and thus results in TNK1-mediated tumor growth in vivo

Published
2021

26. Proteomic Analysis Reveals Sex-Specific Protein Degradation Targets in the Amygdala During Fear Memory Formation

Author

Kayla Farrell, Madeline Musaus, Shaghayegh Navabpour, Kiley Martin, W. Keith Ray, Richard F. Helm, and Timothy J. Jarome

Subjects
Ubiquitin binding, sex difference, Neurosciences. Biological psychiatry. Neuropsychiatry, Protein degradation, Amygdala, UBIQUITIN PROTEASOME SYSTEM, PATHWAY, memory, Cellular and Molecular Neuroscience, Ubiquitin, Western blot, Memory, Protein Degradation Process, ubiquitin, medicine, Fear conditioning, Molecular Biology, Original Research, biology, medicine.diagnostic_test, Neurosciences, RECOGNITION, 1103 Clinical Sciences, amygdala, Cell biology, medicine.anatomical_structure, proteasome, Proteasome, biology.protein, Neurosciences & Neurology, Molecular Neuroscience, 1109 Neurosciences, Life Sciences & Biomedicine, consolidation, RC321-571
Abstract

Ubiquitin-proteasome mediated protein degradation has been widely implicated in fear memory formation in the amygdala. However, to date, the protein targets of the proteasome remain largely unknown, limiting our understanding of the functional significance for protein degradation in fear memory formation. Additionally, whether similar proteins are targeted by the proteasome between sexes has yet to be explored. Here, we combined a degradation-specific K48 Tandem Ubiquitin Binding Entity (TUBE) with liquid chromatography mass spectrometry (LC/MS) to identify the target substrates of the protein degradation process in the amygdala of male and female rats following contextual fear conditioning. We found that males (43) and females (77) differed in the total number of proteins that had significant changes in K48 polyubiquitin targeting in the amygdala following fear conditioning. Many of the identified proteins (106) had significantly reduced levels in the K48-purified samples 1 h after fear conditioning, suggesting active degradation of the substrate due to learning. Interestingly, only 3 proteins overlapped between sexes, suggesting that targets of the protein degradation process may be sex-specific. In females, many proteins with altered abundance in the K48-purified samples were involved in vesicle transport or are associated with microtubules. Conversely, in males, proteins involved in the cytoskeleton, ATP synthesis and cell signaling were found to have significantly altered abundance. Only 1 protein had an opposite directional change in abundance between sexes, LENG1, which was significantly enhanced in males while lower in females. This suggests a more rapid degradation of this protein in females during fear memory formation. Interestingly, GFAP, a critical component of astrocyte structure, was a target of K48 polyubiquitination in both males and females, indicating that protein degradation is likely occurring in astrocytes following fear conditioning. Western blot assays revealed reduced levels of these target substrates following fear conditioning in both sexes, confirming that the K48 polyubiquitin was targeting these proteins for degradation. Collectively, this study provides strong evidence that sex differences exist in the protein targets of the degradation process in the amygdala following fear conditioning and critical information regarding how ubiquitin-proteasome mediated protein degradation may contribute to fear memory formation in the brain. Published version

Published
2021

28. Ubiquitin-binding domain in ABIN1 is critical for regulating cell death and inflammation during development

Author

Jin Bao Li, Qun Zhao, Jianling Liu, Chengxian Xu, Xiaoxia Wu, Han Liu, Jiangshan Deng, Yangjing Ou, Qingfeng Li, Wuwei Rong, Ming Li, Yuwu Zhao, Zhichao Wang, Mingyan Xing, Xiaoming Zhao, Ankang Lv, Xuanhui Wu, Haibing Zhang, Lingxia Wang, Xiuzhe Wang, Yongbo Liu, Xiaoming Li, Fang Li, and Haiwei Zhang

Subjects
Programmed cell death, Ubiquitin binding, Chemistry, medicine, Inflammation, medicine.symptom, Domain (software engineering), Cell biology
Abstract

ABIN1 is a polyubiquitin-binding protein known to regulate NF-κB activation and cell death signaling. Mutations in Abin1 can cause severe immune diseases in human, such as psoriasis, systemic lupus erythematosus, and systemic sclerosis. Here, we generated mice that disrupted the ubiquitin-binding domain of ABIN1 (Abin1UBD/UBD) died during later embryogenesis owing to TNFR1-mediated cell death, similar to Abin1−/− mice. Abin1UBD/UBD cells were rendered sensitive to TNF-α-induced apoptosis and necroptosis as the inhibition of ABIN1UBD and A20 recruitment to the TNF-RSC complex leads to attenuated RIPK1 deubiquitination. Accordingly, the embryonic lethality of Abin1UBD/UBD mice was rescued via crossing with RIPK1 kinase-dead mice (Ripk1K45A/K45A) or the co-deletion of Ripk3 and one allele of Fadd, but not by the loss of Ripk3 or Mlkl alone. Unexpectedly, Abin1UBD/UBD mice with the co-deletion of Ripk3 and both Fadd alleles died at E14.5. This death was caused by spontaneous RIPK1 ubiquitination-dependent multiple inflammatory cytokines over production and could be rescued by the co-deletion of Ripk1 or Tnfr1 combined with Ifnar. Collectively, these data demonstrate the importance of the ABIN1 UBD domain, which mediates the ABIN1-A20 axis, at limiting RIPK1 activation-dependent cell death during embryonic development. Furthermore, our findings reveal a previously unappreciated ubiquitin pathway that regulates cleavage of ubiquitinated RIPK1 by FADD/Casp8 to suppress spontaneous IKK𝜀/TBK1 activation.

Published
2021

29. Quantitative proteomics reveals the selectivity of ubiquitin-binding autophagy receptors in the turnover of damaged lysosomes by lysophagy

Author

J. Wade Harper, Joao A. Paulo, Melissa J Hoyer, Vinay V. Eapen, and Sharan Swarup

Subjects
Proteomics, Autophagosome, autophagy, Ubiquitin binding, QH301-705.5, Science, Quantitative proteomics, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, Biochemistry and Chemical Biology, Lysosome, Macroautophagy, Organelle, medicine, Humans, Biology (General), 030304 developmental biology, Galectin, 0303 health sciences, General Immunology and Microbiology, biology, Chemistry, General Neuroscience, Autophagy, Cell Biology, General Medicine, Cell biology, medicine.anatomical_structure, lysosome, biology.protein, Medicine, cargo receptors, Lysosomes, Flux (metabolism), 030217 neurology & neurosurgery, Protein Binding, Research Article, Human
Abstract

Removal of damaged organelles via the process of selective autophagy constitutes a major form of cellular quality control. Damaged organelles are recognized by a dedicated surveillance machinery, leading to the assembly of an autophagosome around the damaged organelle, prior to fusion with the degradative lysosomal compartment. Lysosomes themselves are also prone to damage and are degraded through the process of lysophagy. While early steps involve recognition of ruptured lysosomal membranes by glycan-binding Galectins and ubiquitylation of transmembrane lysosomal proteins, many steps in the process, and their inter-relationships, remain poorly understood, including the role and identity of cargo receptors required for completion of lysophagy. Here, we employ quantitative organelle capture and proximity biotinylation proteomics of autophagy adaptors, cargo receptors, and Galectins in response to acute lysosomal damage, thereby revealing the landscape of lysosomal proteome remodeling during lysophagy. Among proteins dynamically recruited to damaged lysosomes were ubiquitin-binding autophagic cargo receptors. Using newly developed lysophagic flux reporters including Lyso-Keima, we demonstrate that TAX1BP1, together with its associated kinase TBK1, are both necessary and sufficient to promote lysophagic flux in both Hela cells and induced neurons (iNeurons). While the related receptor OPTN can drive damage-dependent lysophagy when overexpressed, cells lacking either OPTN or CALCOCO2 still maintain significant lysophagic flux in HeLa cells. Mechanistically, TAX1BP1-driven lysophagy requires its N-terminal SKICH domain, which binds both TBK1 and the autophagy regulatory factor RB1CC1, and requires upstream ubiquitylation events for efficient recruitment and lysophagic flux. These results identify TAX1BP1 as a central component in the lysophagy pathway and provide a proteomic resource for future studies of the lysophagy process.

Published
2021

30. The disordered PCI-binding human proteins CSNAP and DSS1 have diverged in structure and function

Author

Sarah F Ruidiaz, Birthe B. Kragelund, Jesper E Dreier, and Rasmus Hartmann-Petersen

Subjects
CANDIDATE GENE, Proteasome Endopeptidase Complex, Magnetic Resonance Spectroscopy, Ubiquitin binding, Full‐Length Papers, IDP, Sequence (biology), Computational biology, REGULATORY PARTICLE, Intrinsically disordered proteins, Biochemistry, Interactome, interactomes, Structure-Activity Relationship, Ubiquitin, CATION-PI INTERACTIONS, Protein Domains, Full‐Length Paper, ubiquitin, Animals, Humans, COP9 signalosome, Molecular Biology, 2-DIMENSIONAL NMR, biology, Chemistry, 26S PROTEASOME, SEM1, signalosome, MESSENGER-RNA EXPORT, NMR, Structure and function, UNSTRUCTURED PROTEINS, Intrinsically Disordered Proteins, proteasome, Proteasome, biology.protein, INTRINSIC DISORDER, Intercellular Signaling Peptides and Proteins, COMPLEXES
Abstract

Intrinsically disordered proteins (IDPs) regularly constitute components of larger protein assemblies contributing to architectural stability. Two small, highly acidic IDPs have been linked to the so-called PCI complexes carrying PCI-domain subunits, including the proteasome lid and the COP9 signalosome. These two IDPs, DSS1 and CSNAP, have been proposed to have similar structural propensities and functions, but they display differences in their interactions and interactome sizes. Here we characterized the structural properties of human DSS1 and CSNAP at the residue level using NMR spectroscopy and probed their propensities to bind ubiquitin. We find that distinct structural features present in DSS1 are completely absent in CSNAP, and vice versa, with lack of relevant ubiquitin binding to CSNAP, suggesting the two proteins to have diverged in both structure and function. Our work additionally highlights that different local features of seemingly similar IDPs, even subtle sequence variance, may endow them with different functional traits. Such traits may underlie their potential to engage in multiple interactions thereby impacting their interactome sizes. This article is protected by copyright. All rights reserved.

Published
2021

31. Bro1 stimulates Vps4 to promote intralumenal vesicle formation during multivesicular body biogenesis

Author

Jennifer Staffenhagen, Ishara F. Azmi, Natalya Pashkova, Johanna A. Payne, Brian A. Davies, Greg Odorizzi, David J. Katzmann, Chun-Che Tseng, Matthew West, Robert C. Piper, and Shirley Dean

Subjects
Organelles, Trafficking, Ubiquitin binding, Endosome, Intralumenal vesicle formation, Vesicle, macromolecular substances, Cell Biology, Biology, Biochemistry, environment and public health, Article, Cell biology, Multivesicular body biogenesis, Ubiquitin, Membrane remodeling, biology.protein, MVB biogenesis
Abstract

Tseng et al. show the Bro1 V domain stimulates Vps4 to promote ESCRT-III–driven intralumenal vesicle formation. This mode of stimulation is required for coordinated cargo incorporation during ESCRT-mediated multivesicular body biogenesis., Endosomal sorting complexes required for transport (ESCRT-0, -I, -II, -III) execute cargo sorting and intralumenal vesicle (ILV) formation during conversion of endosomes to multivesicular bodies (MVBs). The AAA-ATPase Vps4 regulates the ESCRT-III polymer to facilitate membrane remodeling and ILV scission during MVB biogenesis. Here, we show that the conserved V domain of ESCRT-associated protein Bro1 (the yeast homologue of mammalian proteins ALIX and HD-PTP) directly stimulates Vps4. This activity is required for MVB cargo sorting. Furthermore, the Bro1 V domain alone supports Vps4/ESCRT–driven ILV formation in vivo without efficient MVB cargo sorting. These results reveal a novel activity of the V domains of Bro1 homologues in licensing ESCRT-III–dependent ILV formation and suggest a role in coordinating cargo sorting with membrane remodeling during MVB sorting. Moreover, ubiquitin binding enhances V domain stimulation of Vps4 to promote ILV formation via the Bro1–Vps4–ESCRT-III axis, uncovering a novel role for ubiquitin during MVB biogenesis in addition to facilitating cargo recognition.

Published
2021

32. The global proteome and ubiquitinome of bacterial and viral co-infected bronchial epithelial cells

Author

Surabhi Surabhi, Nikolai Siemens, Sven Hammerschmidt, Sandra Maaß, Dörte Becher, and Thomas Sura

Subjects
Proteomics, Ubiquitin binding, Proteome, Mitochondrial translation, Ubiquitin, Biophysics, Pattern recognition receptor, Ubiquitination, Epithelial Cells, Biology, medicine.disease_cause, Biochemistry, Microbiology, Immune system, Host-Pathogen Interactions, Influenza A virus, medicine, biology.protein
Abstract

Viral infections facilitate bacterial trafficking to the lower respiratory tract resulting in bacterial-viral co-infections. Bacterial dissemination to the lower respiratory tract is enhanced by influenza A virus induced epithelial cell damage and dysregulation of immune responses. Epithelial cells act as a line of defense and detect pathogens by a high variety of pattern recognition receptors. The post-translational modification ubiquitin is involved in almost every cellular process. Moreover, ubiquitination contributes to the regulation of host immune responses, influenza A virus uncoating and transport within host cells. We applied proteomics with a special focus on ubiquitination to assess the impact of single bacterial and viral as well as bacterial-viral co-infections on bronchial epithelial cells. We used Tandem Ubiquitin Binding Entities to enrich polyubiquitinated proteins and assess changes in the ubiquitinome. Infecting 16HBE cells with Streptococcus pyogenes led to an increased abundance of proteins related to mitochondrial translation and energy metabolism in proteome and ubiquitinome. In contrast, influenza A virus infection mainly altered the ubiquitinome. Co-infections had no additional impact on protein abundances or affected pathways. Changes in protein abundance and enriched pathways were assigned to imprints of both infecting pathogens. SIGNIFICANCE: Viral and bacterial co-infections of the lower respiratory tract are a burden for health systems worldwide. Therefore, it is necessary to elucidate the complex interplay between the host and the infecting pathogens. Thus, we analyzed the proteome and the ubiquitinome of co-infected bronchial epithelial cells to elaborate a potential synergism of the two infecting organisms. The results presented in this work can be used as a starting point for further analyses.

Published
2021

33. The Extent of Extended-Ubiquitin Binding to the Proteasome

Author

Jeroen Roelofs

Subjects
Proteasome Endopeptidase Complex, 0303 health sciences, Ubiquitin binding, biology, Ubiquitin, Chemistry, 030302 biochemistry & molecular biology, Binding properties, Molecular Conformation, Article, Cell biology, Hop (networking), 03 medical and health sciences, Proteasome, Structural Biology, biology.protein, Receptor, Ubiquitins, Molecular Biology, Protein Binding, 030304 developmental biology
Abstract

Rpn13/Adrm1 is recruited to the proteasome by PSMD1/Rpn2, where it serves as a substrate receptor that binds preferentially to K48-linked ubiquitin chains, an established signal for protein proteolysis. Here, we use NMR to solve the structure of hRpn13 Pru:hRpn2 (940–953):K48-diubiquitin. Surprisingly, hRpn2-bound hRpn13 selects a dynamic, extended conformation of K48-diubiquitin that is unique from previously determined structures. NMR experiments on free K48-diubiquitin demonstrate the presence of the reported ‘closed’ conformation observed by crystallography, but also this more extended state, in which the hRpn13-binding surface is exposed. This extended K48-diubiquitin conformation is defined by interactions between L73 from G76-linked (distal) ubiquitin and a Y59-centered surface of K48-linked (proximal) ubiquitin. Furthermore, hRpn13 exchanges between the two ubiquitins within 100 ms, although prefers the proximal ubiquitin due to interactions with the K48 linker region. Altogether, these data lead to a revised model of how ubiquitinated substrates interact with the proteasome.

Published
2020

34. A20 restricts inflammation via ubiquitin binding

Author

Shao Cong Sun

Subjects
0301 basic medicine, Ubiquitin binding, Immunology, Arthritis, Inflammation, Plasma protein binding, 03 medical and health sciences, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, medicine, Humans, Immunology and Allergy, Ubiquitins, Tumor Necrosis Factor alpha-Induced Protein 3, chemistry.chemical_classification, Mechanism (biology), Arthritis, Psoriatic, medicine.disease, Cell biology, 030104 developmental biology, Enzyme, chemistry, medicine.symptom, Protein Binding, 030215 immunology
Abstract

The ubiquitin-editing enzyme A20 has a pivotal role in restricting autoimmune and inflammatory responses. New studies suggest that A20 prevents inflammatory diseases using a non-catalytic mechanism involving ubiquitin binding.

Published
2020

35. Crosstalk between Lys63- and Lys11-polyubiquitin signaling at DNA damage sites is driven by Cezanne

Author

Mark T. Bedford, David Fushman, Shichang Liu, Bin Wang, Tanuja R. Kashyap, Xiaodong Cheng, Xiao Wu, Cari A. Sagum, Jianji Chen, Rajesh Singh, John R. Horton, and Apurva Chaturvedi

Subjects
0303 health sciences, DNA Repair, biology, Ubiquitin binding, Ubiquitin, DNA damage, DNA repair, Protein domain, Ubiquitination, macromolecular substances, Cell biology, Deubiquitinating enzyme, 03 medical and health sciences, Crosstalk (biology), 0302 clinical medicine, 030220 oncology & carcinogenesis, Genetics, biology.protein, Polyubiquitin, Research Paper, DNA Damage, Protein Binding, 030304 developmental biology, Developmental Biology
Abstract

The establishment of polyubiquitin conjugates with distinct linkages play important roles in the DNA damage response. Much remains unknown about the regulation of linkage-specific ubiquitin signaling at sites of DNA damage. Here we reveal that Cezanne (also known as Otud7B) deubiquitinating enzyme promotes the recruitment of Rap80/BRCA1-A complex by binding to Lys63-polyubiquitin and targeting Lys11-polyubiquitin. Using a ubiquitin binding domain protein array screen, we identify that the UBA domains of Cezanne and Cezanne2 (also known as Otud7A) selectively bind to Lys63-linked polyubiquitin. Increased Lys11-linkage ubiquitination due to lack of Cezanne DUB activity compromises the recruitment of Rap80/BRCA1-A. Cezanne2 interacts with Cezanne, facilitating Cezanne in the recruitment of Rap80/BRCA1-A, Rad18, and 53BP1, in cellular resistance to ionizing radiation and DNA repair. Our work presents a model that Cezanne serves as a “reader” of the Lys63-linkage polyubiquitin at DNA damage sites and an “eraser” of the Lys11-linkage ubiquitination, indicating a crosstalk between linkage-specific ubiquitination at DNA damage sites.

Published
2019

36. The specificity of ubiquitin binding to ubiquilin-1 is regulated by sequences besides its UBA domain

Author

Mervyn J. Monteiro and Christine A. Harman

Subjects
0301 basic medicine, Proteasome Endopeptidase Complex, Ubiquitin binding, Protein subunit, Biophysics, Autophagy-Related Proteins, Protein degradation, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Ubiquitin, Humans, Molecular Biology, Adaptor Proteins, Signal Transducing, biology, Chemistry, Autophagy, Cell biology, 030104 developmental biology, Proteostasis, Proteasome, Proteolysis, biology.protein, Protein folding, 030217 neurology & neurosurgery, Protein Binding
Abstract

UBQLN proteins regulate proteostasis by facilitating clearance of misfolded proteins through the proteasome and autophagy degradation pathways. Consistent with its proteasomal function, UBQLN proteins contain both UBL and UBA domains, which bind subunits of the proteasome, including the S5a subunit, and ubiquitin chains, respectively. Conclusions regarding the binding properties of UBQLN proteins have been derived principally through studies of its individual domains, not the full-length (FL) proteins. Here we describe the in vitro binding properties of FL-UBQLN1 with the S5a subunit of the proteasome and two different lysine-linked (K48 or K63) ubiquitin chains. We show that in contrast to its isolated UBA domain, which binds almost equally well with both K48 and K63 ubiquitin chains, FL UBQLN1 binds preferentially with K63 chains. Furthermore, we show that deletion of the UBL domain from UBQLN1 abrogates ubiquitin binding. Taken together these results suggest that sequences outside of the UBA domain in UBQLN1 function to regulate the specificity and binding with different ubiquitin moieties. We also show that the UBL domain of UBQLN1 is required for S5a binding and that its binding to UBQLN1, in turn, enhances K48 ubiquitin chain binding to the complex. We discuss the implications of our findings with the known function of UBQLN proteins in protein degradation.

Published
2019

37. Identification of a novel EphB4 phosphodegron regulated by the autocrine IGFII/IRA axis in malignant mesothelioma

Author

Vincenzo Carnevale, Pierluigi Scalia, Antonio Giordano, Stephen J Williams, and Giuseppe Pandini

Subjects
0301 basic medicine, Mesothelioma, Cancer Research, Tumor microenvironment, Ubiquitin binding, Angiogenesis, Diagnostic markers, Biology, Receptor tyrosine kinase, Article, 03 medical and health sciences, Insulin receptor, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Genetics, Cancer research, biology.protein, Phosphorylation, Signal transduction, Autocrine signalling, Molecular Biology
Abstract

Malignant mesothelioma is a deadly disease with limited therapeutic options. EphB4 is an oncogenic tyrosine kinase receptor expressed in malignant mesothelioma as well as in a variety of cancers. It is involved in tumor microenvironment mediating angiogenesis and invasive cellular effects via both EphrinB2 ligand-dependent and independent mechanisms. The molecular network underlying EphB4 oncogenic effects is still unclear. Here we show that EphB4 expression in malignant mesothelioma cells is markedly decreased upon neutralization of cancer-secreted IGF-II. In particular, we demonstrate that EphB4 protein expression in malignant mesothelioma cells depend upon a degradation rescue mechanism controlled by the autocrine IGF-II-insulin receptor-A specific signaling axis. We show that the regulation of EphB4 expression is linked to a competing post-translational modification of its carboxy-terminal tail via phosphorylation of its tyrosine 987 by the Insulin receptor isoform-A kinase-associated activity in response to the autocrine IGF-II stimuli. Neutralization of this autocrine-induced EphB4-phosphorylation by IGF-II associates with the increased ubiquitination of EphB4 carboxy-terminal tail and with its rapid degradation. We also describe a novel Ubiquitin binding motif in the targeted region as part of the identified EphB4 phosphodegron and provide 3D modeling data supporting a possible model for the acute EphB4 PTM-driven regulation by IGF-II. Altogether, these findings disclose a novel molecular mechanism for the maintenance of EphB4-expression in malignant mesothelioma cells and other IGF-II-secreting cancers (IGF2omas).

Published
2019

38. A20 prevents inflammasome-dependent arthritis by inhibiting macrophage necroptosis through its ZnF7 ubiquitin-binding domain

Author

Yoshitaka Shirasaki, Bernhard Holzmann, Sotaro Uemura, Marietta Armaka, Manolis Pasparakis, Geert van Loo, Apostolos Polykratis, Masayuki Miura, Arne Martens, Mai Yamagishi, George Kollias, Yoshifumi Yamaguchi, and Remzi Onur Eren

Subjects
Lipopolysaccharides, Programmed cell death, Ubiquitin binding, Inflammasomes, Necroptosis, Inflammatory arthritis, Interleukin-1beta, Kruppel-Like Transcription Factors, Arthritis, Deubiquitinating enzyme, Mice, Necrosis, 03 medical and health sciences, RIPK1, 0302 clinical medicine, immune system diseases, ddc:570, hemic and lymphatic diseases, medicine, Animals, Humans, Tumor Necrosis Factor alpha-Induced Protein 3, 030304 developmental biology, Inflammation, 0303 health sciences, biology, Ubiquitin, Chemistry, Macrophages, NF-kappa B, Inflammasome, Cell Biology, medicine.disease, Cell biology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Mutation, biology.protein, Protein Kinases, Protein Binding, medicine.drug
Abstract

Deficiency in the deubiquitinating enzyme A20 causes severe inflammation in mice, and impaired A20 function is associated with human inflammatory diseases. A20 has been implicated in negatively regulating NF-κB signalling, cell death and inflammasome activation; however, the mechanisms by which A20 inhibits inflammation in vivo remain poorly understood. Genetic studies in mice revealed that its deubiquitinase activity is not essential for A20 anti-inflammatory function. Here we show that A20 prevents inflammasome-dependent arthritis by inhibiting macrophage necroptosis and that this function depends on its zinc finger 7 (ZnF7). We provide genetic evidence that RIPK1 kinase-dependent, RIPK3-MLKL-mediated necroptosis drives inflammasome activation in A20-deficient macrophages and causes inflammatory arthritis in mice. Single-cell imaging revealed that RIPK3-dependent death caused inflammasome-dependent IL-1β release from lipopolysaccharide-stimulated A20-deficient macrophages. Importantly, mutation of the A20 ZnF7 ubiquitin binding domain caused arthritis in mice, arguing that ZnF7-dependent inhibition of necroptosis is critical for A20 anti-inflammatory function in vivo.

Published
2019

39. 1H, 13C and 15N resonance assignments for the tandem CUE domains from chromatin remodeler SMARCAD1

Author

Christina Redfield, Philip West, Erika J. Mancini, and Antonio J. Biasutto

Subjects
0303 health sciences, biology, Ubiquitin binding, Tandem, CUE domain, Heterochromatin, Chemistry, 030303 biophysics, Helicase, Chromatin remodelling, Computational biology, Biochemistry, Article, Chromatin, 03 medical and health sciences, Structural Biology, Secondary structure, NMR resonance assignments, biology.protein, ATPase, Protein secondary structure, 030304 developmental biology, SMARCAD1
Abstract

SMARCAD1 is a non-canonical chromatin remodelling ATPase, unique in its domain organization in that is encodes tandem ubiquitin binding CUE domains along with a classical SNF2 helicase ATP-dependent motor. SMARCAD1 is conserved from yeast to humans and has reported roles in the maintenance of heterochromatin following replication and in double-strand break repair. Here we present the 1H, 13C and 15N assignments for the tandem CUE domains and for the disordered regions that flank them. These assignments provide the starting point for detailed investigations of the structure and interactions of this region of SMARCAD1.

Published
2019

40. Combined Chemical Modification and Collision Induced Unfolding Using Native Ion Mobility-Mass Spectrometry Provides Insights into Protein Gas-Phase Structure

Author

James I. Langridge, David Robinson, Jeddidiah Bellamy-Carter, Neil J. Oldham, Asia Al-jabiry, and Martin Palmer

Subjects
Electrospray, Ubiquitin binding, Ion-mobility spectrometry, Chemistry, Ubiquitin, Organic Chemistry, Chemical modification, General Chemistry, Molecular Dynamics Simulation, Mass spectrometry, Catalysis, Mass Spectrometry, Molecular dynamics, Protein structure, Structural biology, Ion Mobility Spectrometry, Biophysics, Amino Acids
Abstract

Native mass spectrometry is now an important tool in structural biology. Thus, the nature of higher protein structure in the vacuum of the mass spectrometer is an area of significant interest. One of the major goals in the study of gas-phase protein structure is to elucidate the stabilising role of interactions at the level of individual amino acid residues. A strategy combining protein chemical modification together with collision induced unfolding (CIU) was developed and employed to probe the structure of compact protein ions produced by native electrospray ionisation. Tractable chemical modification was used to alter the properties of amino acid residues, and ion mobility-mass spectrometry (IM-MS) utilised to monitor the extent of unfolding as a function of modification. From these data the importance of specific intramolecular interactions for the stability of compact gas-phase protein structure can be inferred. Using this approach, and aided by molecular dynamics simulations, an important stabilising interaction between K6 and H68 in the protein ubiquitin was identified, as was a contact between the N-terminus and E22 in a ubiquitin binding protein UBA2.

Published
2021

41. Structure Activity Relationship of USP5 Allosteric Inhibitors

Author

Rima Al-awar, Taira Kiyota, Matthieu Schapira, M.K. Mann, Carlos Zepeda-Velázquez, Rachel Harding, Ahmed Aman, Cheryl H. Arrowsmith, H.G. Alvarez, and A. Dong

Subjects
chemistry.chemical_classification, Enzyme, Ubiquitin binding, biology, Stereochemistry, Chemistry, Allosteric regulation, biology.protein, Structure–activity relationship, Chemical probe, In vitro, Proto-oncogene tyrosine-protein kinase Src, Deubiquitinating enzyme
Abstract

USP5 is a deubiquitinase that has been implicated in a range of diseases, including cancer, but no USP5-targeting chemical probe has been reported to date. Here, we present the progression of a chemical series that occupies the C-terminal ubiquitin-binding site of a poorly characterized zinc-finger ubiquitin binding domain (ZnF-UBD) of USP5 and allosterically inhibits the catalytic activity of the enzyme. Systematic exploration of the structure-activity relationship, complemented with crystallographic characterization of the ZnF-UBD bound to multiple ligands, led to the identification of 64, which binds to the USP5 ZnF-UBD with a KD of 2.8 µM. 64 is selective over the structurally similar ZnF-UBD domain of HDAC6 and inhibits USP5 catalytic activity in vitro with an IC50 of 26 µM. This study provides a chemical and structural framework for the discovery of a chemical probe to delineate USP5 function in cells. Table of Contents Graphic

Published
2021

42. Molecular recognition and deubiquitination of cyclic K48-linked ubiquitin chains by OTUB1

Author

Daichi Morimoto, Tomoki Sorada, Kenji Sugase, and Erik Walinda

Subjects
0301 basic medicine, Ubiquitin binding, Protein Conformation, Proton Magnetic Resonance Spectroscopy, Biophysics, Cleavage (embryo), Biochemistry, Deubiquitinating enzyme, 03 medical and health sciences, 0302 clinical medicine, Molecular recognition, Ubiquitin, Humans, Molecular Biology, chemistry.chemical_classification, biology, Deubiquitinating Enzymes, Nitrogen Isotopes, Lysine, Ubiquitination, Cell Biology, Kinetics, 030104 developmental biology, Enzyme, chemistry, OTUB1, Cyclization, 030220 oncology & carcinogenesis, biology.protein, Deubiquitination
Abstract

Conjugation of K48-linked ubiquitin chains to intracellular proteins mainly functions as a signal for proteasomal degradation. The conjugating enzyme E2-25K synthesizes not only canonical (noncyclic) but also cyclic K48-linked ubiquitin chains. Although the cyclic conformation is expected to repress molecular recognition by ubiquitin binding proteins due to restricting the flexibility of the ubiquitin subunits in a chain, multiple proteins are reported to associate with cyclic ubiquitin chains similar to noncyclic chains. However, the molecular mechanism of how cyclic ubiquitin chains are recognized remains unclear. Here we investigated the effect of cyclization on ubiquitin-chain cleavage and molecular recognition by a K48-linkage specific deubiquitinating enzyme OTUB1 for cyclic diubiquitin by NMR spectroscopic analyses. Compared to noncyclic diubiquitin, we observed slow but unambiguously detectable cleavage of cyclic diubiquitin to monoubiquitin by OTUB1. Intriguingly, upon ubiquitin chain cleavage, cyclic diubiquitin appeared to alter its "autoinhibited" conformation to an incompletely but partially accessible conformation, induced by interaction with OTUB1 via the ubiquitin-subunit specific recognition patches and adjacent surfaces. These data imply that cyclic ubiquitin chains may exist stably in cells in spite of the presence of deubiquitinating enzymes and that these chains can be recognized by intracellular proteins in a manner distinct from that of noncyclic ubiquitin chains.

Published
2021

44. Expression and clinical significance of UBE2V1 in cervical cancer

Author

Zhendong Liu, Zhishuai Ren, Shenqian Ma, Ruiya Wang, Yanzheng Gao, Junming Yue, Jinming Yang, and Yuqi Guo

Subjects
Cervical cancer, biology, Ubiquitin binding, business.industry, QH301-705.5, Biophysics, Methylation, QD415-436, Biomarker, medicine.disease, Biochemistry, Real-time polymerase chain reaction, Ubiquitin, Oncology, DNA methylation, biology.protein, medicine, Cancer research, Biomarker (medicine), Clinical significance, Biology (General), UBE2V1, business, Research Article
Abstract

The majority of cervical cancer (CC) patients are caused by the high-risk human papillomavirus (HPV) infection Although they are preventable and controllable, the mortality rate is still high. It is essential to identify the biomarkers for early screening and diagnosis of CC to improve the prognosis of patients with CC. The conjugating enzyme 2 (E2) family members are the key components of ubiquitin protease system. However, the role of E2 family in CC remains unclear. We aimed to investigate the role of UBE2V1, a ubiquitin binding E2 enzyme variant protein (ube2v) without conserved cysteine residues required for E2s catalytic activity in CC. In this study, we first studied the expression of UBE2V1 in CC by real time quantitative PCR (RT-qPCR), and then, the clinical information of 191 CC patients in TCGA database was retrieved to explore the relationship between the expression of UBE2V1 and the occurrence and development of CC by examining the translational profile and methylation, the high expression of UBE2V1 was well correlated to the poor prognosis of patients, indicating that UBE2V1 is an independent risk factor for the prognosis of CC patients. The expression of UBE2V1 was also correlated with clinical stages, tumor grades and TNM stages of CC. In addition, the expression of UBE2V1 was slightly negatively correlated with the methylation at the multiple methylation sites. our study revealed the relationship between UBE2V1 and the occurrence and development of CC from the level of transcriptional profile and DNA methylation. UBE2V1 is a novel candidate biomarker for the diagnosis, screening and prognosis of CC., Highlights • The expression of UBE2V1 was abnormal in cervical cancer. • UBE2V1 is associated with poor prognosis in patients with cervical cancer. • UBE2V1 can be used as a new tumor marker for cervical cancer.

Published
2021

45. TEX264 at the intersection of autophagy and DNA repair

Author

John Fielden, Marta Popović, and Kristijan Ramadan

Subjects
0301 basic medicine, Nucleophagy, Ubiquitin binding, DNA Repair, DNA repair, Valosin-containing protein, ATG8, Review, 03 medical and health sciences, Autophagy, TEX264, autophagy, GyrI proteins, p97, Molecular Biology, Mechanistic target of rapamycin, Phylogeny, 030102 biochemistry & molecular biology, biology, Ubiquitin, Cell Biology, Autophagy-Related Protein 8 Family, DNA, Endoplasmic Reticulum Stress, Cell biology, Ubiquitin ligase, RING finger domain, 030104 developmental biology, biology.protein
Abstract

TEX264 (testes expressed gene 264) is a single-pass transmembrane protein, consisting of an N-terminal hydrophobic region, a gyrase inhibitory (GyrI)-like domain, and a loosely structured C terminus. TEX264 was first identified as an endoplasmic reticulum (ER)-resident Atg8-family-binding protein that mediates the degradation of portions of the ER during starvation (i.e., reticulophagy). More recently, TEX264 was identified as a cofactor of VCP/p97 ATPase that promotes the repair of covalently trapped TOP1 (DNA topoisomerase 1)-DNA crosslinks. This review summarizes the current knowledge of TEX264 as a protein with roles in both autophagy and DNA repair and provides an evolutionary and structural analysis of GyrI proteins. Based on our phylogenetic analysis, we provide evidence that TEX264 is a member of a large superfamily of GyrI-like proteins that evolved in bacteria and are present in metazoans, including invertebrates and chordates.Abbreviations: Atg8: autophagy related 8; Atg39: autophagy related 39; Cdc48: cell division cycle 48; CGAS: cyclic GMP-AMP synthase; DPC: DNA-protein crosslinks; DSB: DNA double-strand break; ER: endoplasmic reticulum; GyrI: gyrase inhibitory domain; LRR: leucine-rich repeat; MAFFT: multiple alignment using fast Fourier transform; MAP1LC3/LC3: microtubule-associated protein 1 light chain 3; MTOR: mechanistic target of rapamycin kinase; STUBL: SUMO targeted ubiquitin ligase; SUMO: small ubiquitin-like modifier; TEX264: testis expressed gene 264; TOP1cc: topoisomerase 1-cleavage complex; UBZ: ubiquitin binding Zn finger domain; VCP: valosin containing protein.

Published
2021

46. PS-341 alleviates chronic low-grade inflammation and improves insulin sensitivity through the inhibition of TM4 (UBAC2) degradation

Author

Li Yintao, Zhen Yang, Min He, Qiwei Shen, Kuanping Ye, Lili Chen, Bin Lu, Rumei Li, Wenbai Zhou, Jinya Huang, Zhaoyun Zhang, Qin Li, Lianxi Li, Yehong Yang, Qiyuan Yao, Jie Wen, Cheng Hu, Feng Xiaocheng, Xuanchun Wang, Naijia Liu, Ying Huang, Qinghua Wang, and Renming Hu

Subjects
UBAC2, medicine.medical_specialty, RC620-627, Nerve growth factor IB, Ubiquitin binding, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Inflammation, Clinical nutrition, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Downregulation and upregulation, In vivo, Internal medicine, Medicine, TX341-641, Obesity, Nutritional diseases. Deficiency diseases, 030304 developmental biology, 0303 health sciences, Nutrition and Dietetics, business.industry, Nutrition. Foods and food supply, Research, medicine.disease, PS-341, Metabolic inflammation, Endocrinology, 030220 oncology & carcinogenesis, medicine.symptom, business
Abstract

Background The TM4 (UBAC2) protein, which contains 4 transmembrane domains and one ubiquitin binding domain, is mainly expressed in cell and nuclear membranes. The current research aimed to explore the role of TM4 in metabolic inflammation and to examine whether the ubiquitin–proteasome inhibitor PS-341 could regulate the function of TM4. Methods The metabolic phenotypes of TM4 knockout (KO) mice were studied. We next explored the association between the polymorphisms of TM4 and obesity in a Chinese Han population. TM4 expression in the visceral fat of obese patients who underwent laparoscopic cholecystectomy was also analysed. Finally, the effect of PS-341 on the degradation and function of the TM4 protein was investigated in vivo and in vitro. Results TM4 KO mice developed obesity, hepatosteatosis, hypertension, and glucose intolerance under a high-fat diet. TM4 counterregulated Nur77, IKKβ, and NF-kB both in vivo and in vitro. The TM4 SNP rs147851454 is significantly associated with obesity after adjusting for age and sex (OR 1.606, 95% CI 1.065–2.422 P = 0.023) in 3394 non-diabetic and 1862 type 2 diabetic adults of Han Chinese. TM4 was significantly downregulated in the visceral fat of obese patients. PS-341 induced TM4 expression through inhibition of TM4 degradation in vitro. In db/db mice, PS-341 administration led to downregulation of Nur77/IKKβ/NF-κB expression in visceral fat and liver, and alleviation of hyperglycaemia, hypertension, and glucose intolerance. The hyperinsulinaemic-euglycaemic clamp demonstrated that PS-341 improved the glucose infusion rate and alleviated insulin resistance in db/db mice. Conclusions PS-341 alleviates chronic low-grade inflammation and improves insulin sensitivity through inhibition of TM4 degradation.

Published
2021

47. Mechanism of activation and regulation of Deubiquitinase activity in MINDY1 and MINDY2

Author

Knebel, Abdul Rehman, Lange, Grawert, Svergun, Kulathu, Kristariyanto, and Armstrong

Subjects
chemistry.chemical_classification, Deubiquitinase activity, Substrate Interaction, Enzyme, Ubiquitin binding, Ubiquitin, biology, Chemistry, Stereochemistry, Catalytic triad, biology.protein, Substrate (chemistry), Cleavage (embryo)
Abstract

Of the eight distinct polyubiquitin chains that can be assembled, K48-linked ubiquitin is the most well-understood linkage and modification of proteins with K48 chains targets the modified protein for degradation. By removing ubiquitin from substrates or trimming ubiquitin chains, deubiquitinases (DUBs) can modulate the outcome of ubiquitylation. MINDY1 and MINDY2 are members of the MINDY family of DUBs that have exquisite specificity for cleaving K48-linked polyubiquitin. Being recently discovered DUBs, we have a poor understanding of their catalytic mechanism. By analysing crystal structures of MINDY1 alone and in complex with monoubiquitin or K48-linked ubiquitin chains, we here reveal how substrate interaction relieves autoinhibition and activates the DUB. Further, our analyses reveal a non-canonical catalytic triad composed of Cys-His-Thr and explain how these DUBs sense both ubiquitin chain length and linkage type to trim K48-linked ubiquitin chains. Our findings highlight the multiple layers of regulation modulating DUB activity in MINDY1 and MINDY2.SynopsisStructure of MINDY1 in complex with K48-linked diUb reveals how K48-linked polyUb is recognized and cleavedThe Cys loop mediates autoinhibition of the DUB and substrate binding at the S1 and S1’ sites relieves autoinhibition and activates the enzyme for catalysisMINDY1 uses a non-canonical catalytic triad composed of Cys-His-ThrMINDY1 has five ubiquitin binding sites within its catalytic domain and switches from exo to endo cleavage in a ubiquitin chain length-dependent manner

Published
2021

48. Tandem Ubiquitin Binding Entities (TUBEs) as Tools to Explore Ubiquitin-Proteasome System and PROTAC Drug Discovery

Author

Myra J Zerr, Karteek Kadimisetty, Dahmane Ouazia, Patrick H Gross, and Katie J Sheets

Subjects
Ubiquitin binding, biology, Chemistry, Drug discovery, Protein domain, macromolecular substances, Protein degradation, environment and public health, Cell biology, Blot, Proteasome, Ubiquitin, biology.protein, Target protein
Abstract

The ubiquitin proteasome system (UPS) is a complex pathway that involves multiple enzymes and culminates in the formation of a polyubiquitin chain on a target protein. As its importance is becoming more evident in drug discovery, there is a renewed interest in understanding the role that polyubiquitin chains play. This has been a challenge, mostly due to the lack of experimental tools for detecting the polyubiquitinated forms of a protein of interest (POI). Tandem Ubiquitin Binding Entities (TUBEs) are engineered protein domains that bind specifically to polyubiquitin chains. These polyubiquitin affinity matrices are highly sensitive as they bind to polyubiquitin chains in the nanomolar range. They exist in two forms: pan-selective TUBEs and chain-selective TUBEs. The ability of TUBEs to be conjugated to different entities is truly what makes them unique. TUBEs are used in a wide variety of experiments such as in protein pulldowns to enrich for polyubiquitinated proteins. They are an alternative to ubiquitin antibodies in Western blots. Further, TUBEs are used as capture reagents for immobilizing polyubiquitinated proteins on a microtiter plate. The use of TUBEs as components of in vitro and cell-based assays presents the unique feature of confirming and assessing the polyubiquitination of a POI in response to inhibitors, activators, or PROTAC® molecules. Therefore, TUBEs not only play a big role in studying the UPS but also have a huge potential for speeding up the drug discovery process.

Published
2021

49. The nuclear localization sequence of the epigenetic factor RYBP binds to human importin α3

Author

Adrián Velázquez-Campoy, Bruno Rizzuti, Ana Jiménez-Alesanco, José L. Neira, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Diputación General de Aragón, and Centro de Investigación Biomédica en Red Enfermedades Hepáticas y Digestivas (España)

Subjects
0301 basic medicine, alpha Karyopherins, Magnetic Resonance Spectroscopy, Ubiquitin binding, Nuclear Localization Signals, Biophysics, Importin, Calorimetry, Karyopherins, environment and public health, Biochemistry, Analytical Chemistry, Epigenesis, Genetic, 03 medical and health sciences, NLS, Humans, Amino Acid Sequence, Binding site, Molecular Biology, Cell Nucleus, Binding Sites, 030102 biochemistry & molecular biology, Chemistry, Binding protein, RYBP, Nuclear Proteins, Isothermal titration calorimetry, Intrinsically Disordered Proteins, Molecular Docking Simulation, Repressor Proteins, Protein Transport, 030104 developmental biology, Peptide, Nuclear localization sequence, Nuclear location signal, Binding domain, Protein Binding
Abstract

13 pags, 9 figs. -- Supplementary data to this article can be found online at https://doi.org/10.1016/j.bbapap.2021.140670., RYBP (Ring1 and YY1 binding protein, UniProt ID: Q8N488) is an epigenetic factor with a key role during embryonic development; it does also show an apoptotic function and an ubiquitin binding activity. RYBP is an intrinsically disordered protein (IDP), with a Zn-finger domain at its N-terminal region, which folds upon binding to DNA. It is predicted that RYBP has a nuclear localization sequence (NLS), comprising residues Asn58 to Lys83, to allow for nuclear translocation. We studied in this work the ability of intact RYBP to bind Impα3 and its truncated species, ΔImpα3, without the importin binding domain (IBB), by using fluorescence and circular dichroism (CD). Furthermore, the binding of the peptide matching the isolated NLS region of RYBP (NLS-RYBP) was also studied using the same methods and isothermal titration calorimetry (ITC), and in silico molecular docking. Moreover, we carried out experiments with NLS-RYBP in the absence or in the presence of NaCl (140 mM). Our results show that RYBP interacted with Impα3 and ΔImpα3, causing protein precipitation. The NLS-RYBP also interacted with both importin species (dissociation constant in the low micromolar range), at low or high ionic strength, as shown by intrinsic fluorescence and ITC. These findings indicate that the NLS region, which was mainly unfolded in isolation in solution, was essentially responsible for the binding of RYBP to each of the importin species. Furthermore, the molecular simulations predict that the anchoring of NLS-RYBP takes place in the major binding site for the NLS of cargo proteins bound to Impα3. Taken together, our findings pinpoint the theoretical predictions of the NLS region in RYBP and, more importantly, suggest that this IDP relies on an importin for its nuclear translocation., The authors thank two anonymous reviewers for helpful suggestions and discussions. BR acknowledges the kind use of computational resources of the European Magnetic Resonance Center (CERM), Sesto Fiorentino (Florence), Italy. This research was funded by Spanish Ministry of Economy and Competitiveness and European ERDF Funds (MCIU/AEI/FEDER, EU) [RTI2018-097991-B-I00 to JLN and BFU2016-78232-P to AVC]; Diputacion General de Aragon [Protein Targets and Bioactive Compounds Group E45_17R to AVC and Pre-doctoral Research Contract 2019 to AJA]; and Centro de Investigacion Biomedica en Red en Enfermedades Hepaticas y Digestivas (CIBERehd). JLN thanks Miguel Vidal (CIB, CSIC, Madrid) for the kindly gift of the RYBP vector.

Published
2020

50. The Structure and Ubiquitin Binding Properties of TRAF RING Heterodimers

Author

Anubrita Das, Adam J. Middleton, Catherine L. Day, Elizabeth C. Ledgerwood, Prasanth Padala, and Peter D. Mace

Subjects
TRAF3, Ubiquitin binding, Architecture domain, Ubiquitin-Protein Ligases, Ring (chemistry), Receptors, Tumor Necrosis Factor, Protein–protein interaction, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, Structural Biology, Humans, Protein Interaction Domains and Motifs, Molecular Biology, 030304 developmental biology, Zinc finger, TNF Receptor-Associated Factor 6, 0303 health sciences, TNF Receptor-Associated Factor 5, biology, TNF Receptor-Associated Factor 3, Chemistry, Ubiquitination, Zinc Fingers, TNF Receptor-Associated Factor 2, Cell biology, biology.protein, Linker, Dimerization, 030217 neurology & neurosurgery, Protein Binding, Signal Transduction
Abstract

Tumour necrosis factor (TNF) receptor associated factor (TRAF) family members share a common domain architecture, but play non-redundant physiological roles in cell signalling. At the N terminus, most TRAFs have a RING domain, followed by a series of Zinc finger (ZF) domains. The RING domain of TRAF6 dimerizes, and the RING homodimer together with the first ZF assembles ubiquitin chains that form a platform which facilitates activation of downstream kinases. The RING dimer interface is conserved amongst TRAF proteins, suggesting that functional heterodimers could be possible. Here we report the structure of the TRAF5-TRAF6 RING heterodimer, which accounts for the stability of the heterodimer as well as its ability to assemble ubiquitin chains. We also show that the RING domain of TRAF6 heterodimerizes with TRAF3 and TRAF2, and demonstrate that the linker helix and first ZF of TRAF2 can cooperate with TRAF6 to promote chain assembly. Collectively our results suggest that TRAF RING homo- and hetero-dimers have the potential to bridge interaction of nearby TRAF trimers and modulate TRAF-mediated signalling.

Published
2020

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