Your search keyword '"Fuchs SY"' showing total 14 results

1. Type I interferon controls propagation of long interspersed element-1.

Author

Yu Q, Carbone CJ, Katlinskaya YV, Zheng H, Zheng K, Luo M, Wang PJ, Greenberg RA, and Fuchs SY

Subjects

Animals, Embryo, Mammalian, Fibroblasts cytology, Fibroblasts immunology, Gene Expression Regulation, Genomic Instability, HeLa Cells, Humans, Interferon-alpha immunology, Interferon-alpha metabolism, Interferon-beta immunology, Interferon-beta metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, NIH 3T3 Cells, Primary Cell Culture, RNA Helicases deficiency, RNA Helicases genetics, RNA Helicases immunology, Receptor, Interferon alpha-beta deficiency, Receptor, Interferon alpha-beta genetics, Receptor, Interferon alpha-beta immunology, Signal Transduction, Testis cytology, Testis immunology, Testis metabolism, Fibroblasts metabolism, Interferon-alpha genetics, Interferon-beta genetics, Long Interspersed Nucleotide Elements

Abstract

Type I interferons (IFN) including IFNα and IFNβ are critical for the cellular defense against viruses. Here we report that increased levels of IFNβ were found in testes from mice deficient in MOV10L1, a germ cell-specific RNA helicase that plays a key role in limiting the propagation of retrotransposons including Long Interspersed Element-1 (LINE-1). Additional experiments revealed that activation of LINE-1 retrotransposons increases the expression of IFNβ and of IFN-stimulated genes. Conversely, pretreatment of cells with IFN suppressed the replication of LINE-1. Furthermore, the efficacy of LINE-1 replication was increased in isogenic cell lines harboring inactivating mutations in diverse elements of the IFN signaling pathway. Knockdown of the IFN receptor chain IFNAR1 also stimulated LINE-1 propagation in vitro. Finally, a greater accumulation of LINE-1 was found in mice that lack IFNAR1 compared with wild type mice. We propose that LINE-1-induced IFN plays an important role in restricting LINE-1 propagation and discuss the putative role of IFN in preserving the genome stability., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

2. Tyrosine phosphorylation of protein kinase D2 mediates ligand-inducible elimination of the Type 1 interferon receptor.

Author

Zheng H, Qian J, Baker DP, and Fuchs SY

Subjects

Antiviral Agents pharmacology, Enzyme Activation drug effects, Enzyme Activation genetics, HeLa Cells, Humans, Interferon-alpha pharmacology, Phosphorylation drug effects, Phosphorylation physiology, Protein Kinase D2, Protein Kinases genetics, Protein Structure, Tertiary, Receptor, Interferon alpha-beta genetics, TYK2 Kinase genetics, TYK2 Kinase metabolism, Tyrosine genetics, Tyrosine metabolism, Protein Kinases metabolism, Receptor, Interferon alpha-beta immunology

Abstract

Type 1 interferons (including IFNα/β) activate their cell surface receptor to induce the intracellular signal transduction pathways that play an important role in host defenses against infectious agents and tumors. The extent of cellular responses to IFNα is limited by several important mechanisms including the ligand-stimulated and specific serine phosphorylation-dependent degradation of the IFNAR1 chain of Type 1 IFN receptor. Previous studies revealed that acceleration of IFNAR1 degradation upon IFN stimulation requires activities of tyrosine kinase TYK2 and serine/threonine protein kinase D2 (PKD2), whose recruitment to IFNAR1 is also induced by the ligand. Here we report that activation of PKD2 by IFNα (but not its recruitment to the receptor) depends on TYK2 catalytic activity. PKD2 undergoes IFNα-inducible tyrosine phosphorylation on specific phospho-acceptor site (Tyr-438) within the plekstrin homology domain. Activated TYK2 is capable of facilitating this phosphorylation in vitro. Tyrosine phosphorylation of PKD2 is required for IFNα-stimulated activation of this kinase as well as for efficient serine phosphorylation and degradation of IFNAR1 and ensuing restriction of the extent of cellular responses to IFNα.

Published

2011

3. Role of p38 protein kinase in the ligand-independent ubiquitination and down-regulation of the IFNAR1 chain of type I interferon receptor.

Author

Bhattacharya S, Qian J, Tzimas C, Baker DP, Koumenis C, Diehl JA, and Fuchs SY

Subjects

Animals, Gene Knockdown Techniques, HeLa Cells, Humans, Interferon-alpha metabolism, Interferon-alpha pharmacology, Interferon-beta metabolism, Interferon-beta pharmacology, Ligands, Mice, Phosphorylation drug effects, Phosphorylation genetics, Protein Kinase Inhibitors pharmacology, Protein Stability drug effects, Signal Transduction drug effects, Signal Transduction genetics, Vesiculovirus physiology, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors, p38 Mitogen-Activated Protein Kinases deficiency, p38 Mitogen-Activated Protein Kinases genetics, Down-Regulation drug effects, Down-Regulation genetics, Receptor, Interferon alpha-beta metabolism, Ubiquitination drug effects, Ubiquitination genetics, p38 Mitogen-Activated Protein Kinases metabolism

Abstract

Phosphorylation-dependent ubiquitination and degradation of the IFNAR1 chain of type I interferon (IFN) receptor is a robust and specific mechanism that limits the magnitude and duration of IFNα/β signaling. Besides the ligand-inducible IFNAR1 degradation, the existence of an "inside-out" signaling that accelerates IFNAR1 turnover in the cells undergoing the endoplasmic reticulum (ER) stress and activated unfolded protein responses has been recently described. The latter pathway does not require either presence of ligands (IFNα/β) or catalytic activity of Janus kinases (JAK). Instead, this pathway relies on activation of the PKR-like ER kinase (PERK) and ensuing specific priming phosphorylation of IFNAR1. Here, we describe studies that identify the stress activated p38 protein kinase as an important regulator of IFNAR1 that acts downstream of PERK. Results of the experiments using pharmacologic p38 kinase inhibitors, RNA interference approach, and cells from p38α knock-out mice suggest that p38 kinase activity is required for priming phosphorylation of IFNAR1 in cells undergoing unfolded protein response. We further demonstrate an important role of p38 kinase in the ligand-independent stimulation of IFNAR1 ubiquitination and degradation and ensuing attenuation of IFNα/β signaling and anti-viral defenses. We discuss the distinct importance of p38 kinase in regulating the overall responses to type I IFN in cells that have been already exposed to IFNα/β versus those cells that are yet to encounter these cytokines.

Published

2011

4. Inducible priming phosphorylation promotes ligand-independent degradation of the IFNAR1 chain of type I interferon receptor.

Author

Bhattacharya S, HuangFu WC, Liu J, Veeranki S, Baker DP, Koumenis C, Diehl JA, and Fuchs SY

Subjects

Amino Acid Sequence, Animals, Casein Kinase I metabolism, Conserved Sequence, Fibroblasts cytology, HeLa Cells, Humans, Immunologic Factors metabolism, Immunologic Factors pharmacology, Interferon-alpha metabolism, Interferon-alpha pharmacology, Interferon-beta metabolism, Interferon-beta pharmacology, Ligands, Mice, Molecular Sequence Data, Phosphorylation physiology, Receptor, Interferon alpha-beta genetics, Signal Transduction drug effects, Ubiquitin-Protein Ligases metabolism, Unfolded Protein Response physiology, eIF-2 Kinase metabolism, Receptor, Interferon alpha-beta metabolism, Signal Transduction physiology, Ubiquitination physiology

Abstract

Phosphorylation-dependent ubiquitination and ensuing down-regulation and lysosomal degradation of the interferon alpha/beta receptor chain 1 (IFNAR1) of the receptor for Type I interferons play important roles in limiting the cellular responses to these cytokines. These events could be stimulated either by the ligands (in a Janus kinase-dependent manner) or by unfolded protein response (UPR) inducers including viral infection (in a manner dependent on the activity of pancreatic endoplasmic reticulum kinase). Both ligand-dependent and -independent pathways converge on phosphorylation of Ser(535) within the IFNAR1 degron leading to recruitment of beta-Trcp E3 ubiquitin ligase and concomitant ubiquitination and degradation. Casein kinase 1 alpha (CK1 alpha) was shown to directly phosphorylate Ser(535) within the ligand-independent pathway. Yet given the constitutive activity of CK1 alpha, it remained unclear how this pathway is stimulated by UPR. Here we report that induction of UPR promotes the phosphorylation of a proximal residue, Ser(532), in a pancreatic endoplasmic reticulum kinase-dependent manner. This serine serves as a priming site that promotes subsequent phosphorylation of IFNAR1 within its degron by CK1 alpha. These events play an important role in regulating ubiquitination and degradation of IFNAR1 as well as the extent of Type I interferon signaling.

Published

2010

5. Basal ubiquitin-independent internalization of interferon alpha receptor is prevented by Tyk2-mediated masking of a linear endocytic motif.

Author

Kumar KG, Varghese B, Banerjee A, Baker DP, Constantinescu SN, Pellegrini S, and Fuchs SY

Subjects

Amino Acid Motifs physiology, Cell Line, Humans, Multiprotein Complexes genetics, Multiprotein Complexes metabolism, Receptor, Interferon alpha-beta genetics, TYK2 Kinase genetics, Ubiquitin genetics, Ubiquitin metabolism, Down-Regulation physiology, Endocytosis physiology, Receptor, Interferon alpha-beta metabolism, Signal Transduction physiology, TYK2 Kinase metabolism, Ubiquitination physiology

Abstract

Linear endocytic motifs of signaling receptors as well as their ubiquitination determine the rate of ligand-induced endocytosis that mediates down-regulation of these receptors and restricts the magnitude and duration of their respective signal transduction pathways. We previously hypothesized that, in the absence of its cognate ligand, type I interferon (IFN), the IFNalpha receptor chain 1 (IFNAR1) receptor chain is protected from basal endocytosis by a hypothetical masking complex that prevents the Tyr-based endocytic motif within IFNAR1 from interacting with components of the adaptin protein complex 2 (AP2). Here we identify a member of the Janus kinase (Jak) family, Tyk2, as a component of such a masking complex. In the absence of ligand or of receptor chain ubiquitination, binding of Janus kinase Tyk2 within the proximity of the Tyr-based linear motif of IFNAR1 is required to prevent IFNAR1 internalization and to maintain its cell surface expression. Furthermore, interaction experiments revealed that Tyk2 physically shields this Tyr-based motif from the recognition by the AP50 subunit of AP2. These data delineate a long-sought ligand- and ubiquitin-independent mechanism by which Tyk2 contributes to both the regulation of total IFNAR1 levels as well as the regulation of the cell surface density of this receptor chain.

Published

2008

6. Phosphorylation and specific ubiquitin acceptor sites are required for ubiquitination and degradation of the IFNAR1 subunit of type I interferon receptor.

Author

Kumar KG, Krolewski JJ, and Fuchs SY

Subjects

Amino Acid Motifs, Binding Sites, Cell Line, Cytoplasm metabolism, HeLa Cells, Humans, Immunoblotting, Immunoprecipitation, Ligands, Lysine chemistry, Lysosomes metabolism, Membrane Proteins, Phosphorylation, Plasmids metabolism, Protein Binding, Protein Structure, Tertiary, Protein-Tyrosine Kinases metabolism, Receptor, Interferon alpha-beta, Serine chemistry, TYK2 Kinase, Time Factors, Receptors, Interferon chemistry, Ubiquitin metabolism

Abstract

Ubiquitination, endocytosis, and lysosomal degradation of the IFNAR1 (interferon alpha receptor 1) subunit of the type I interferon (IFN) receptor is mediated by the SCFbeta-Trcp (Skp1-Cullin1-F-box protein beta transducin repeat-containing protein) E3 ubiquitin ligase in a phosphorylation-dependent manner. In addition, stability of IFNAR1 is regulated by its binding to Tyk2 kinase. Here we characterize the determinants of IFNAR1 ubiquitination and degradation. We found that the integrity of two Ser residues at positions 535 and 539 within the specific destruction motif present in the cytoplasmic tail of IFNAR1 is essential for the ability of IFNAR1 to recruit beta-Trcp as well as to undergo efficient ubiquitination and degradation. Using an antibody that specifically recognizes IFNAR1 phosphorylated on Ser535 we found that IFNAR1 is phosphorylated on this residue in cells. This phosphorylation is promoted by treatment of cells with IFNalpha. Although the cytoplasmic tail of IFNAR1 contains seven Lys residues that could function as potential ubiquitin acceptor sites, we found that only three (Lys501, Lys525, and Lys526), all located proximal to the destruction motif, are essential for ubiquitination and degradation of IFNAR1. Expression of Tyk2 stabilized IFNAR1 in a manner that was dependent neither on its binding to beta-Trcp nor IFNAR1 ubiquitination. We discuss the complexities and specifics of the ubiquitination and degradation of IFNAR1, which is a beta-Trcp substrate that undergoes degradation via a lysosomal pathway.

Published

2004

7. Stability of homologue of Slimb F-box protein is regulated by availability of its substrate.

Author

Li Y, Gazdoiu S, Pan ZQ, and Fuchs SY

Subjects

Base Sequence, Cell Line, Cysteine Endopeptidases metabolism, DNA Damage, DNA Primers, Humans, Hydrolysis, Multienzyme Complexes metabolism, Mutation, Proteasome Endopeptidase Complex, Proteins chemistry, Proteins genetics, Substrate Specificity, Ubiquitin metabolism, Proteins metabolism

Abstract

The homologue of Slimb (HOS) F-box protein is a receptor of the Skp1-Cullin1-F-box protein (SCF(HOS)) E3 ubiquitin ligase, which mediates ubiquitination and degradation of beta-catenin and the inhibitor of NFkappaB, IkappaB. We found that HOS itself is an unstable protein that undergoes ubiquitination and degradation in a 26 S proteasome-dependent manner. A HOS mutant lacking the F-box that is deficient in binding to the core SCF components underwent ubiquitination less efficiently and was more stable than the wild type protein. Furthermore, ubiquitination and degradation of HOS was impaired in ts41 cells, in which the activities of Cullin-based ligases were decreased because the NEDD8 pathway was abrogated. Whereas HOS was directly ubiquitinated within the SCF(HOS) complex in vitro, the addition of phosphorylated IkappaBalpha inhibited this ubiquitination. Increasing cellular levels of HOS substrate (phosphorylated IkappaBalpha) by activating IkappaB kinase inhibited HOS ubiquitination and led to stabilization of HOS, indicating that interaction between HOS and its substrate might protect HOS from proteolysis. Taken together, our data suggest that proteolysis of HOS depends on its interaction with active components of the SCF complex and that HOS stability is regulated by a bound substrate. These findings may define a mechanism for maintaining activities of specific SCF complexes based on availability of a particular substrate.

Published

2004

8. Interaction of Epstein-Barr virus latent membrane protein 1 with SCFHOS/beta-TrCP E3 ubiquitin ligase regulates extent of NF-kappaB activation.

Author

Tang W, Pavlish OA, Spiegelman VS, Parkhitko AA, and Fuchs SY

Subjects

Amino Acid Sequence, Animals, Cell Line, Humans, Hydrolysis, Molecular Sequence Data, Phosphorylation, Rats, Viral Matrix Proteins genetics, NF-kappa B metabolism, Ubiquitin-Protein Ligases metabolism, Viral Matrix Proteins metabolism

Abstract

The Epstein-Barr virus latent membrane protein 1 (LMP1) is pivotal in the transforming activity of this virus. We found that the common LMP1-95-8 variant interacts with Homologue of Slimb (HOS), a receptor for the SCFHOS/betaTrCP ubiquitin-protein isopeptide ligase (E3) via one canonical and one cryptic HOS recognition site. These sites are mutated or deleted in the tumor-derived LMP1-Cao variant, which did not bind to HOS. Mutations within these sites on LMP1-95-8 abrogated HOS binding and increased transforming activity of LMP1. HOS did not regulate stability of LMP1-95-8 unless it was mutated to bear additional lysine residues near the cryptic motif. LMP1 proteins that could not bind to HOS exhibited an increased ability to induce IkappaB degradation and NF-kappaB-mediated transcription without further increase in activation of IkappaB kinases. Expression of LMP1-95-8 reduced the levels of endogenous HOS available to interact with phosphorylated IkappaBalpha. Degradation of IkappaBalpha and dose dependence of NF-kappaB activation by LMP1-95-8 were promoted by co-expression of HOS. Our data suggest that LMP1-95-8 is a pseudo-substrate of SCFHOS/betaTrCP E3 ubiquitin ligase and that interaction between LMP1 and HOS restricts the extent of LMP1-induced NF-kappaB signaling. We discuss the potential role of this mechanism in transforming and cytostatic effects of LMP1 variants in cells and Epstein-Barr virus-associated tumors.

Published

2003

9. Induction of homologue of Slimb ubiquitin ligase receptor by mitogen signaling.

Author

Spiegelman VS, Tang W, Chan AM, Igarashi M, Aaronson SA, Sassoon DA, Katoh M, Slaga TJ, and Fuchs SY

Subjects

3T3 Cells, Animals, Blotting, Northern, Cell Differentiation, Cell Nucleus metabolism, Cell Transformation, Neoplastic, Dose-Response Relationship, Drug, Down-Regulation, Enzyme Activation, Fibroblasts metabolism, Genes, Dominant, Humans, Immunoblotting, Mice, NF-kappa B metabolism, Ornithine Decarboxylase metabolism, Precipitin Tests, Signal Transduction, Time Factors, Tumor Cells, Cultured, Ligases metabolism, Mitogens metabolism, Ubiquitin metabolism

Abstract

Homologue of Slimb (HOS) is the substrate-recognizing component of the SCF(HOS)-Roc1 E3 ubiquitin protein ligase. This ligase mediates ubiquitination of the inhibitor of NF-kappaB transcription factor (IkappaB). We have found that HOS is highly expressed in a number of human cancer cell lines. The rates of the HOS gene transcription as well as HOS mRNA and protein levels were up-regulated in cells treated with mitogens or transfected with the inducers of mitogen-activated protein kinase pathway. Conversely, mitogen withdrawal strikingly reduced HOS levels during differentiation of mouse myoblasts. Activators of mitogen-activated protein kinase accelerated IkappaBalpha degradation and increased NF-kappaB transcriptional activity. Inhibition of HOS function via expression of dominant negative HOS (HOS(DeltaF)) initiated mouse myoblast differentiation and prevented Ras-mediated acceleration of IkappaBalpha degradation as well as NF-kappaB trans-activation and transformation of NIH3T3 cells. These data link the induction of HOS in proliferating cells with mitogen-signaling-dependent inhibition of cell differentiation and promotion of cell transformation.

Published

2002

10. Induction of beta-transducin repeat-containing protein by JNK signaling and its role in the activation of NF-kappaB.

Author

Spiegelman VS, Stavropoulos P, Latres E, Pagano M, Ronai Z, Slaga TJ, and Fuchs SY

Subjects

3T3 Cells, Amino Acid Sequence, Animals, Cell Line, GTP-Binding Proteins genetics, Humans, JNK Mitogen-Activated Protein Kinases, Mice, Molecular Sequence Data, RNA, Messenger chemistry, RNA, Messenger genetics, beta-Transducin Repeat-Containing Proteins, GTP-Binding Proteins biosynthesis, Mitogen-Activated Protein Kinases metabolism, NF-kappa B metabolism, Signal Transduction

Abstract

Activation of Jun N-kinase (JNK) and NF-kappaB transcription factor are the hallmarks of cellular response to stress. Phosphorylation of NF-kappaB inhibitor (IkappaB) by respective stress-inducible kinases (IKK) is a key event in NF-kappaB activation. beta-TrCP F-box protein mediates ubiquitination of phosphorylated IkappaB via recruitment of SCF(beta-TrCP)-Roc1 E3 ubiquitin ligase complex. Subsequent proteasome-dependent degradation of IkappaB results in activation of the NF-kappaB pathway. We found that a variety of cellular stress stimuli induce an increase in the steady state levels of beta-TrCP mRNA and protein levels in human cells. Activation of stress-activated protein kinases JNK (and, to a lesser extent, p38) by forced expression of constitutively active mutants of JNKK2 and MKK6 (but not MEK1 or IKKbeta) also leads to accumulation of beta-TrCP. Transcription of the beta-TrCP gene is not required for JNK-mediated induction of beta-TrCP. A synergistic effect of stimulation of IKK and JNK on the transcriptional activity of NF-kappaB was observed. The mechanisms of beta-TrCP induction via stress and its role in NF-kappaB activation are discussed.

Published

2001

11. Stabilization and activation of p53 by the coactivator protein TAFII31.

Author

Buschmann T, Lin Y, Aithmitti N, Fuchs SY, Lu H, Resnick-Silverman L, Manfredi JJ, Ronai Z, and Wu X

Subjects

3T3 Cells, Animals, Blotting, Northern, Blotting, Western, Cell Cycle, Cell Division, Fibroblasts metabolism, Flow Cytometry, Genes, Reporter, Genes, p53 genetics, Genetic Vectors, Mice, Mice, Inbred BALB C, Mutation, Plasmids metabolism, Precipitin Tests, Protein Binding, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-mdm2, Suppression, Genetic, Transcription, Genetic, Transcriptional Activation, Transfection, Ubiquitins metabolism, Ultraviolet Rays, Gene Expression Regulation, Nuclear Proteins, TATA-Binding Protein Associated Factors, Trans-Activators metabolism, Transcription Factor TFIID, Tumor Suppressor Protein p53 metabolism

Abstract

Regulation of the stability of p53 is key to its tumor-suppressing activities. mdm2 directly binds to the amino-terminal region of p53 and targets it for degradation through the ubiquitin-proteasome pathway. The coactivator protein TAF(II)31 binds to p53 at the amino-terminal region that is also required for interaction with mdm2. In this report, we demonstrate that expression of TAF(II)31 inhibits mdm2-mediated ubiquitination of p53 and increases p53 levels. TAF(II)31-mediated p53 stabilization results in activation of p53-mediated transcriptional activity and leads to p53-dependent growth arrest in fibroblasts. UV-induced stabilization of p53 coincides with an increase in p53-associated TAF(II)31 and a corresponding decrease in mdm2-p53 interaction. Non-p53 binding mutant of TAF(II)31 fails to stabilize p53. Our results suggest that direct interaction of TAF(II)31 and p53 not only mediates p53 transcriptional activation but also protects p53 from mdm2-mediated degradation, thereby resulting in activation of p53 functions.

Published

2001

12. The conserved RING-H2 finger of ROC1 is required for ubiquitin ligation.

Author

Chen A, Wu K, Fuchs SY, Tan P, Gomez C, and Pan ZQ

Subjects

Amino Acid Sequence, Amino Acid Substitution, Anaphase-Promoting Complex-Cyclosome, Animals, Binding Sites, Cell Line, Conserved Sequence, Cysteine, Humans, Hydroxymercuribenzoates pharmacology, Kinetics, Ligases antagonists & inhibitors, Mercuric Chloride pharmacology, Mice, Mutagenesis, Site-Directed, Protein Conformation, Recombinant Fusion Proteins metabolism, Sulfhydryl Reagents pharmacology, Transfection, Ubiquitin-Conjugating Enzymes, Ubiquitin-Protein Ligases, Ligases chemistry, Ligases metabolism, Ubiquitin-Protein Ligase Complexes, Ubiquitins metabolism

Abstract

ROC1 is a common component of a large family of ubiquitin E3 ligases that regulate cell cycle progression and signal transduction pathways. Here we present evidence suggesting that a conserved RING-H2 structure within ROC1 is critical for its ubiquitin ligation function. Mercury-containing sulfhydryl modification agents (rho-hydroxymercuribenzoate and mercuric chloride) irreversibly inhibit the ROC1-CUL1 ubiquitin ligase activity without disrupting the complex. Consistent with this, these reagents also eliminate the ability of the Skp1-CUL1-HOS-ROC1 E3 ligase complex to support the ubiquitination of IkappaBalpha. Site-directed mutagenesis analysis identifies RING-H2 finger residues Cys(42), Cys(45), Cys(75), His(77), His(80), Cys(83), Cys(94), and Asp(97) as being essential for the ROC1-dependent ubiquitin ligase activity. Furthermore, C42S/C45S and H80A mutations reduce the ability of ROC1 to interact with CUL1 in transfected cells and diminish the capacity of ROC1-CUL1 to form a stable complex with Cdc34 in vitro. However, C75S, H77A, C94S, and D97A substitutions have no detectable effect on ROC1 binding activities. Thus, the ROC1 RING-H2 finger may possess multiple biochemical properties that include stabilizing an interaction with CUL1 and recruiting Cdc34. A possible role of the RING finger in facilitating the Ub transfer reaction is discussed.

Published

2000

13. Stability of the ATF2 transcription factor is regulated by phosphorylation and dephosphorylation.

Author

Fuchs SY, Tappin I, and Ronai Z

Subjects

Activating Transcription Factor 2, Cell Line, Fibroblasts metabolism, Humans, MAP Kinase Signaling System, Models, Biological, Okadaic Acid pharmacology, Phosphorylation, Plasmids, Protein Serine-Threonine Kinases metabolism, Time Factors, Trans-Activators metabolism, Transfection, Tumor Necrosis Factor-alpha metabolism, Ubiquitins metabolism, Calcium-Calmodulin-Dependent Protein Kinases physiology, Cyclic AMP Response Element-Binding Protein metabolism, MAP Kinase Kinase Kinase 1, Transcription Factors metabolism

Abstract

Trans-activation of the activating transcription factor-2 (ATF2) in response to cellular stress requires the N-terminal phosphorylation of ATF2 by stress-activated protein kinases (SAPK). In this study, we investigated the role of ATF2 phosphorylation in the maintenance of ATF2 stability. Activation of SAPK by forced expression of DeltaMEKK1 increased overall ATF2 ubiquitination, presumably because of the enhanced dimerization of ATF2. Treatment of DeltaMEKK1-expressing cells with okadaic acid led to the increase in N-terminal phosphorylation, protection from ubiquitination, and accumulation of exogenously expressed ATF2, indicating the role of protein phosphatases in balancing the effects of stress kinases. Analysis of ubiquitination and degradation of the constitutively dimerized ATF2 mutant (ATF2(Delta150-248)) showed that activation of JNK or p38 kinase renders ATF2 resistant to ubiquitination and degradation. This effect is mediated by JNK/p38-dependent phosphorylation of ATF2 at Thr-69 and Thr-71, because the phosphorylation-deficient mutant (ATF2(Delta150-248-T69A,T71A)) was not protected from ubiquitination and degradation by the activation of SAPK. Treatment of cells with okadaic acid elevated the tumor necrosis factor alpha-induced ATF2 level and the extent of its specific N-terminal phosphorylation. Cycloheximide, which activates SAPK, while inhibiting protein synthesis, stabilized endogenous ATF2. However, treatment of cells with the high dose of SB203580, which inhibits JNK and p38 kinase, resulted in efficient degradation of ATF2 in cells exposed to cycloheximide. This degradation was abrogated by co-treatment with the proteasome inhibitor MG132. Our findings suggest that N-terminal phosphorylation of ATF2 dimers protect ATF2 from ubiquitination and degradation. We propose the hypothesis that the balance between SAPK and protein phosphatases affects the duration and magnitude of ATF2 transcriptional output because of the effect on substrate recognition for ubiquitination and degradation.

Published

2000

14. c-Jun NH2-terminal kinases target the ubiquitination of their associated transcription factors.

Author

Fuchs SY, Xie B, Adler V, Fried VA, Davis RJ, and Ronai Z

Subjects

3T3 Cells, Activating Transcription Factor 2, Animals, Cysteine Endopeptidases metabolism, Hydrolysis, JNK Mitogen-Activated Protein Kinases, Mice, Multienzyme Complexes metabolism, Phosphorylation, Proteasome Endopeptidase Complex, Proto-Oncogene Proteins metabolism, Substrate Specificity, ets-Domain Protein Elk-1, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Cyclic AMP Response Element-Binding Protein metabolism, DNA-Binding Proteins, Mitogen-Activated Protein Kinases, Proto-Oncogene Proteins c-jun metabolism, Transcription Factors metabolism, Ubiquitins metabolism

Abstract

Regulatory proteins are often ubiquitinated, depending on their phosphorylation status as well as on their association with ancillary proteins that serve as adapters of the ubiquitination machinery. We previously demonstrated that c-Jun is targeted for ubiquitination by its association with inactive c-Jun NH2-terminal kinase (JNK). Phosphorylation by activated JNK protects c-Jun from ubiquitination, thus by prolonging its half-life. In the study reported here, we determined the ability of JNK to target ubiquitination of its other substrates (Elk1 and activating transcription factor 2 (ATF2)) and associated proteins (ATF2 and JunB). We demonstrate that phosphorylation by JNK protects ATF2, but not Elk1, from JNK-targeted ubiquitination. We also show that association of inactive JNK with JunB or ATF2 is necessary to target them for ubiquitination. Unlike its targeting of c-Jun, JNK requires additional cellular components, yet to be identified, to target the ubiquitination of ATF2. Elk1 is phosphorylated by JNK, but JNK neither associates with nor targets Elk1 for ubiquitination. The implications for the dual role of JNK in the regulation of ubiquitination and stability of c-Jun, ATF2, and JunB in normally growing versus stressed cells are discussed.

Published

1997