Your search keyword '"Ubiquitins biosynthesis"' showing total 7 results

1. ISG15 is a critical microenvironmental factor for pancreatic cancer stem cells.

Author

Sainz B Jr, Martín B, Tatari M, Heeschen C, and Guerra S

Subjects

Biomarkers, Tumor, Carcinoma, Pancreatic Ductal pathology, Cytokines biosynthesis, Gene Expression Regulation, Neoplastic, Humans, Macrophages metabolism, Neoplasm Metastasis, Neoplastic Stem Cells metabolism, Tumor Microenvironment genetics, Ubiquitins biosynthesis, Carcinogenesis genetics, Carcinoma, Pancreatic Ductal genetics, Cytokines genetics, Neoplastic Stem Cells pathology, Ubiquitins genetics

Abstract

Cancer stem cells (CSC) are thought to play a major role in the development and metastatic progression of pancreatic ductal adenocarcinoma (PDAC), one of the deadliest solid tumors. Likewise, the tumor microenvironment contributes critical support in this setting, including from tumor stromal cells and tumor-associated macrophages (TAM) that contribute structural and paracrine-mediated supports, respectively. Here, we show that TAMs secrete the IFN-stimulated factor ISG15, which enhances CSC phenotypes in PDAC in vitro and in vivo. ISG15 was preferentially and highly expressed by TAM present in primary PDAC tumors resected from patients. ISG15 was secreted by macrophages in response to secretion of IFNβ by CSC, thereby reinforcing CSC self-renewal, invasive capacity, and tumorigenic potential. Overall, our work demonstrates that ISG15 is a previously unrecognized support factor for CSC in the PDAC microenvironment with a key role in pathogenesis and progression., (©2014 American Association for Cancer Research.)

Published

2014

2. BRCA1 ubiquitinates RPB8 in response to DNA damage.

Author

Wu W, Nishikawa H, Hayami R, Sato K, Honda A, Aratani S, Nakajima T, Fukuda M, and Ohta T

Subjects

Cell Line, Tumor, Epirubicin pharmacology, HeLa Cells, Humans, Protein Subunits, Tumor Suppressor Proteins metabolism, Ubiquitin-Protein Ligases metabolism, Ubiquitins biosynthesis, Ultraviolet Rays, BRCA1 Protein metabolism, DNA Damage physiology, DNA-Directed RNA Polymerases metabolism

Abstract

The breast and ovarian tumor suppressor BRCA1 catalyzes untraditional polyubiquitin chains that could be a signal for processes other than proteolysis. However, despite intense investigations, the mechanisms regulated by the enzyme activity remain only partially understood. Here, we report that BRCA1-BARD1 mediates polyubiquitination of RPB8, a common subunit of RNA polymerases, in response to DNA damage. A proteomics screen identified RPB8 as a protein modified after epirubicin treatment in BRCA1-dependent manner. RPB8 interacted with BRCA1-BARD1 and was polyubiquitinated by BRCA1-BARD1 in vivo and in vitro. BRCA1-BARD1 did not destabilize RPB8 in vivo but rather caused an increase in the amount of soluble RPB8. Importantly, RPB8 was polyubiquitinated immediately after UV irradiation in a manner sensitive to BRCA1 knockdown by RNA interference. Substitution of five lysine residues of RPB8 with arginine residues abolished its ability to be ubiquitinated while preserving its polymerase activity. HeLa cell lines stably expressing this ubiquitin-resistant form of RPB8 exhibited UV hypersensitivity accompanied by up-regulated caspase activity. Our findings suggest that ubiquitination of a common subunit of RNA polymerases is a mechanism underlying BRCA1-dependent cell survival after DNA damage.

Published

2007

3. Transforming growth factor-beta, estrogen, and progesterone converge on the regulation of p27Kip1 in the normal and malignant endometrium.

Author

Lecanda J, Parekh TV, Gama P, Lin K, Liarski V, Uretsky S, Mittal K, and Gold LI

Subjects

Adult, Cell Growth Processes physiology, Cell Nucleus metabolism, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p27, Cytoplasm metabolism, Endometrial Neoplasms enzymology, Endometrial Neoplasms pathology, Endothelium cytology, Endothelium drug effects, Endothelium enzymology, Endothelium metabolism, Female, Humans, Intracellular Signaling Peptides and Proteins genetics, Middle Aged, Mitogen-Activated Protein Kinases metabolism, RNA, Messenger biosynthesis, RNA, Messenger genetics, Tumor Cells, Cultured, Ubiquitins biosynthesis, Endometrial Neoplasms metabolism, Estradiol pharmacology, Intracellular Signaling Peptides and Proteins metabolism, Progesterone pharmacology, Transforming Growth Factor beta pharmacology

Abstract

Hormones and growth factors regulate endometrial cell growth. Disrupted transforming growth factor-beta (TGF-beta) signaling in primary endometrial carcinoma (ECA) cells leads to loss of TGF-beta-mediated growth inhibition, which we show herein results in lack of up-regulation of the cyclin-dependent kinase inhibitor p27(Kip1) (p27) to arrest cells in G(1) phase of the cell cycle. Conversely, in normal primary endometrial epithelial cells (EECs), TGF-beta induces a dose-dependent increase in p27 protein, with a total 3.6-fold maximal increase at 100 pmol/L TGF-beta, which was 2-fold higher in the nuclear fraction; mRNA levels were unaffected. In addition, ECA tissue lysates show a high rate of ubiquitin-mediated degradation of p27 compared with normal secretory-phase endometrial tissue (SE) such that 4% and 89% of recombinant p27 added to the lysates remains after 3 and 20 h, respectively. These results are reflected in vivo as ECA tissue lacks p27 compared with high expression of p27 in SE (P < or = 0.001). Furthermore, we show that estrogen treatment of EECs causes mitogen-activated protein kinase-driven proteasomal degradation of p27 whereas progesterone induces a marked increase in p27 in both normal EECs and ECA cells. Therefore, these data suggest that TGF-beta induces accumulation of p27 for normal growth regulation of EECs. However, in ECA, in addition to enhanced proteasomal degradation of p27, TGF-beta cannot induce p27 levels due to dysregulated TGF-beta signaling, thereby causing 17beta-estradiol-driven p27 degradation to proceed unchecked for cell cycle progression. Thus, p27 may be a central target for growth regulation of normal endometrium and in the pathogenesis of ECA.

Published

2007

4. Elevated expression of ISG15 in tumor cells interferes with the ubiquitin/26S proteasome pathway.

Author

Desai SD, Haas AL, Wood LM, Tsai YC, Pestka S, Rubin EH, Saleem A, Nur-E-Kamal A, and Liu LF

Subjects

Breast Neoplasms genetics, Breast Neoplasms pathology, Cell Transformation, Neoplastic, Female, Gene Expression Profiling, Humans, Proteins metabolism, RNA, Small Interfering, Tumor Cells, Cultured, Ubiquitins biosynthesis, Ubiquitins physiology, Up-Regulation, Cytokines biosynthesis, Cytokines physiology, Proteasome Endopeptidase Complex metabolism, Ubiquitin metabolism

Abstract

IFN-stimulatory gene factor 15 (ISG15) is a ubiquitin-like protein, which is conjugated to many cellular proteins. However, its role in protein degradation is unclear. Here, we show that ISG15 is highly elevated and extensively conjugated to cellular proteins in many tumors and tumor cell lines. The increased levels of ISG15 in tumor cells were found to be associated with decreased levels of polyubiquitinated proteins. Specific knockdown of ISG15 expression using ISG15-specific small interfering RNA (siRNA) was shown to increase the levels of polyubiquitinated proteins, suggesting an antagonistic role of ISG15 in regulating ubiquitin-mediated protein turnover. Moreover, siRNA-mediated down-regulation of the major E2 for ISG15 (UbcH8), which blocked the formation of ISG15 protein conjugates, also increased the levels of polyubiquitinated proteins. Together, our results suggest that the ISG15 pathway, which is deregulated during tumorigenesis, negatively regulates the ubiquitin/proteasome pathway by interfering with protein polyubiquitination/degradation.

Published

2006

5. Myristoylation of the fus1 protein is required for tumor suppression in human lung cancer cells.

Author

Uno F, Sasaki J, Nishizaki M, Carboni G, Xu K, Atkinson EN, Kondo M, Minna JD, Roth JA, and Ji L

Subjects

Animals, Carcinoma, Non-Small-Cell Lung genetics, Cell Line, Tumor, Genes, Tumor Suppressor, Humans, Lung Neoplasms genetics, Mice, Mice, Nude, Protein Precursors biosynthesis, Protein Precursors genetics, Subcellular Fractions metabolism, Tumor Suppressor Proteins, Ubiquitins biosynthesis, Ubiquitins genetics, Carcinoma, Non-Small-Cell Lung metabolism, Lung Neoplasms metabolism, Myristic Acid metabolism, Protein Precursors metabolism, Protein Processing, Post-Translational, Ubiquitins metabolism

Abstract

FUS1 is a novel tumor suppressor gene identified in the human chromosome 3p21.3 region that is deleted in many cancers. Using surface-enhanced laser desorption/ionization mass spectrometric analysis on an anti-Fus1-antibody-capture ProteinChip array, we identified wild-type Fus1 as an N-myristoylated protein. N-myristoylation is a protein modification process in which a 14-carbon myristoyl group is cotranslationally and covalently added to the NH2-terminal glycine residue of the nascent polypeptide. Loss of expression or a defect of myristoylation of the Fus1 protein was observed in human primary lung cancer and cancer cell lines. A myristoylation-deficient mutant of the Fus1 protein abrogated its ability to inhibit tumor cell-induced clonogenicity in vitro, to induce apoptosis in lung tumor cells, and to suppress the growth of tumor xenografts and lung metastases in vivo and rendered it susceptible to rapid proteasome-dependent degradation. Our results show that myristoylation is required for Fus1-mediated tumor-suppressing activity and suggest a novel mechanism for the inactivation of tumor suppressors in lung cancer and a role for deficient posttranslational modification in tumor suppressor-gene-mediated carcinogenesis.

Published

2004

6. Protein metabolism in the small intestine during cancer cachexia and chemotherapy in mice.

Author

Samuels SE, Knowles AL, Tilignac T, Debiton E, Madelmont JC, and Attaix D

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma metabolism, Animals, Antineoplastic Agents pharmacology, Atrophy, Blotting, Northern, Cachexia etiology, Cathepsin B biosynthesis, Cathepsin B genetics, Cathepsin B metabolism, Colonic Neoplasms drug therapy, Colonic Neoplasms metabolism, Eating, Gene Expression, Intestine, Small drug effects, Intestine, Small pathology, Male, Mice, Mice, Inbred BALB C, Neoplasm Transplantation, Nitrosourea Compounds pharmacology, Protein Biosynthesis, Ubiquitins biosynthesis, Ubiquitins genetics, Ubiquitins metabolism, Adenocarcinoma complications, Antineoplastic Agents toxicity, Cachexia metabolism, Colonic Neoplasms complications, Intestine, Small metabolism, Nitrosourea Compounds toxicity, Proteins metabolism

Abstract

The impact of cancer cachexia and chemotherapy on small intestinal protein metabolism and its subsequent recovery was investigated. Cancer cachexia was induced in mice with colon 26 adenocarcinoma, which is a small and slow-growing tumor characteristic of the human condition, and can be cured with 100% efficacy using an experimental nitrosourea, cystemustine (C6H12ClN3O4S). Both healthy mice and tumor-bearing mice were given a single i.p. injection of cystemustine (20 mg/kg) 3 days after the onset of cachexia. Cancer cachexia led to a reduced in vivo rate of protein synthesis in the small intestine relative to healthy mice (-13 to -34%; P < 0.05), resulting in a 25% loss of protein mass (P < 0.05), and decreased villus width and crypt depth (P < 0.05). In treated mice, acute cytotoxicity of chemotherapy did not promote further wasting of small intestinal protein mass, nor did it result in further damage to intestinal morphology. In contrast, mucosal damage and a 17% reduction in small intestinal protein mass (P < 0.05) were evident in healthy mice treated with cystemustine, suggesting that the effects of chemotherapy on the small intestine in a state of cancer cachexia are not additive, which was an unexpected finding. Complete and rapid recovery of small intestinal protein mass in cured mice resulted from an increase in the rate of protein synthesis compared with healthy mice (23-34%; P < 0.05). Northern hybridizations of mRNA encoding components of the major proteolytic systems suggested that proteolysis may not have mediated intestinal wasting or recovery. A major clinical goal should be to design methods to improve small intestinal protein metabolism before the initiation of chemotherapy.

Published

2000

7. Elevation of interferon beta-inducible proteins in ataxia telangiectasia cells.

Author

Siddoo-Atwal C, Haas AL, and Rosin MP

Subjects

Antibodies pharmacology, Ataxia Telangiectasia pathology, Cell Line, Fibroblasts metabolism, Gene Expression Regulation, Humans, Interferon-beta genetics, Interferon-beta immunology, NF-kappa B physiology, Neutralization Tests, Ubiquitins biosynthesis, Ataxia Telangiectasia metabolism, Cysteine Endopeptidases, Cytokines, Interferon-beta biosynthesis, Protein Biosynthesis, Ubiquitins analogs & derivatives

Abstract

The recently cloned ATM gene has been shown to bear considerable homology to phosphatidylinositol 3 kinases and, therefore, its product may function in signal transduction. In this study, we report constitutively elevated levels of two IFN-beta-inducible proteins, ubiquitin cross-reactive protein (UCRP), and low molecular weight protein (LMP2), in human fibroblasts with the inherited disease ataxia telangiectasia (AT). Using immunoblotting, it was found that a M(r) 15,000 band representing free UCRP was hardly detectable in normal cells, while it was the predominant band in AT cells. Similarly, the expression of a M(r) 23,000 protein, LMP2 was found to be higher in AT cells than in normal cells. Culturing three successive passages of the AT cell line in the presence of different concentrations of neutralizing antibodies against IFN-beta caused partial and complete reduction, respectively, of the free UCRP and LMP2 signals to normal levels. These results indicate that UCRP and LMP2 pools may be basally elevated in AT cells due to constitutive activation of the IFN-beta induction pathway and are in keeping with the recently reported constitutive activation of the NF-kappaB transcriptional activator in AT cells.

Published

1996