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483 results on '"Upstream Stimulatory Factor"'

1. USF1 Silencing Reduces Ferroptosis Resistance in Prostate Cancer Cells.

Author

Gao L and Li J

Subjects
Humans, Male, Cell Line, Tumor, Tumor Cells, Cultured, Neoplasm Invasiveness genetics, Ferroptosis genetics, Upstream Stimulatory Factors genetics, Upstream Stimulatory Factors metabolism, Prostatic Neoplasms genetics, Prostatic Neoplasms pathology, Prostatic Neoplasms metabolism, Gene Silencing
Abstract

Background: Ferroptosis is an iron-dependent cell death mode. Ferroptosis resistance is related to prostate cancer (PCa) invasion; However, there is vague understanding with regard to the underlying mechanism. This study was undertaken to clarify the role and mechanism of upstream stimulatory factor 1 ( USF1 ) in ferroptosis resistance in invasive PCa., Methods: USF1 was silenced in the human PCa cell lines C4-2B and PC-3. After these cells were treated with a ferroptosis inhibitor, cell viability and invasion and the expression of glutathione peroxidase 4 (GPX4) were evaluated. Chromatin immunoprecipitation and Dual-luciferase reporter assay suggested an interaction between USF1 and brain-expressed X-linked protein 1 ( BEX1 ). Consequently, BEX1 was overexpressed in USF1 -silenced C4-2B and PC-3 cells and its effects on cell viability and invasion and GPX4 expression were examined., Results: USF1 silencing mitigated PCa cell viability and invasion. Treatment with a ferroptosis inhibitor counteracted the inhibitory roles of USF1 silencing in cell invasion and GPX4 expression. Additionally, USF1 silencing decreased BEX1 expression and USF1 was found to bind to the BEX1 promoter. BEX1 overexpression reversed the influences of USF1 silencing on the viability, BEX1 protein expression, invasive ability and ferroptosis of PCa cells., Conclusions: USF1 activates the transcription of BEX1 , preventing PCa cell ferroptosis and promoting cell invasion. Therefore, USF1 silencing may inhibit the progression of PCa by reducing ferroptosis resistance., Competing Interests: The authors declare no conflict of interest., (© 2024 The Author(s).)

Published
2024
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2. Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs.

Author

Moss, Charlotte E., Johnston, Simon A., Kimble, Joshua V., Clements, Martha, Codd, Veryan, Hamby, Stephen, Goodall, Alison H., Deshmukh, Sumeet, Sudbery, Ian, Coca, Daniel, Wilson, Heather L., and Kiss-Toth, Endre

Abstract

Macrophages are central innate immune cells whose function declines with age. The molecular mechanisms underlying age-related changes remain poorly understood, particularly in human macrophages. We report a substantial reduction in phagocytosis, migration, and chemotaxis in human monocyte-derived macrophages (MDMs) from older (>50 years old) compared with younger (18–30 years old) donors, alongside downregulation of transcription factors MYC and USF1. In MDMs from young donors, knockdown of MYC or USF1 decreases phagocytosis and chemotaxis and alters the expression of associated genes, alongside adhesion and extracellular matrix remodeling. A concordant dysregulation of MYC and USF1 target genes is also seen in MDMs from older donors. Furthermore, older age and loss of either MYC or USF1 in MDMs leads to an increased cell size, altered morphology, and reduced actin content. Together, these results define MYC and USF1 as key drivers of MDM age-related functional decline and identify downstream targets to improve macrophage function in aging. [Display omitted] • Human monocyte and macrophage migration and phagocytosis is markedly reduced with age • MYC and USF1 are driving this aged macrophage phenotype in both human and murine cells • MYC- and USF1-regulated pathways are potential targets for therapeutic intervention Moss et al. report that human monocytes and monocyte-derived macrophages have a marked reduction in migration and phagocytosis. This aged macrophage phenotype is driven by master-regulator transcription factors MYC and USF1 in both human and murine cells, providing a strong platform for identification of pathways and targets for intervention studies. [ABSTRACT FROM AUTHOR]

Published
2024
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10. The Structure and Function of the Adenovirus Major Late Promoter

Author

Young, C. S. H., Compans, R. W., editor, Cooper, M. D., editor, Ito, Y., editor, Koprowski, H., editor, Melchers, F., editor, Oldstone, M. B. A., editor, Olsnes, S., editor, Potter, M., editor, Vogt, P. K., editor, Wagner, H., editor, Doerfler, Walter, editor, and Böhm, Petra, editor

Published
2003
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14. A novel protein upstream stimulatory factor 2 identified in lamprey, Lethenteron reissneri

Author

Peng Su, Qingwei Li, Tiesong Li, Yue Pang, and Yuxuan Guo

Subjects
Fish Proteins, 0106 biological sciences, 0301 basic medicine, Leucine zipper, Subfamily, Transcription, Genetic, Protein Conformation, Amino Acid Motifs, USF2, USF1, 010603 evolutionary biology, 01 natural sciences, Upstream Stimulatory Factor, Evolution, Molecular, 03 medical and health sciences, Genetics, Animals, Gene family, Amino Acid Sequence, Gene, Conserved Sequence, Phylogeny, biology, Helix-Loop-Helix Motifs, Immunity, Lampreys, Exons, Open reading frame, 030104 developmental biology, biology.protein, Upstream Stimulatory Factors, Transcription Factors, Developmental Biology
Abstract

Upstream stimulatory factors are kinds of multi-functional transcription factors, which are expressed in eukaryotes widely, including Upstream stimulatory factor 1 (USFl) and upstream stimulatory factor 2 (USF2). USF protein has a typical basic helix-loop-helix leucine zipper (b-HLH-LZ) structure, which is involved in cell cycle, cell proliferations, glucose and lipid metabolism, and other biochemical processes. Although the USF family is an important regulator of cellular processes, little is known about the USF genes of lampreys, especially their evolutionary relationships, expression profiles, and biological functions. Here, an upstream stimulatory factor 2 (USF2) homolog from lamprey (Lethenteron reissneri) was identified and characterized (designated as L-USF2) because it is closer to USF2 subfamily than to USF1 subfamily. The cDNA fragment of L-USF2 has an open reading frame (ORF) of 765-bp length, encodes 254 amino acids, and contains an HLH domain at the c-terminal of amino acids. Meanwhile, motifs and genetic structure analysis reveal that USF2 gene exons are conserved. Moreover, the 3D structure analysis indicates that L-USF2 adopts the general USF2 folding and has a high structural similarity with H-USF2. The synteny results showed that the L-USF2 adjacent gene changed greatly compared with the jaw vertebrates. By real-time quantitative experiment and Western blot analysis, we found that L-USF2 gene played a significant role in the immune responses. This study not only provides us with a further understanding of the evolution and function of the USF gene family but also provides a basis for exploring its immune responses and immune defenses in lampreys.

Published
2020

17. Myc/Max Family of Transcription Factors and bcl-2 are Involved in Drug-induced Apoptosis of Myeloma Cells

Author

Siegel, D. S., Terry, J. A., Koury, J., Barlogie, B., Epstein, J., Feinman, R., Compans, R. W., editor, Cooper, M., editor, Hogle, J. M., editor, Koprowski, H., editor, Ito, Y., editor, Melchers, F., editor, Oldstone, M., editor, Olsnes, S., editor, Potter, M., editor, Saedler, H., editor, Vogt, P. K., editor, Wagner, H., editor, Potter, Michael, editor, and Melchers, Fritz, editor

Published
1997
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22. U

Author

Rieger, R., Michaelis, A., Green, M. M., Rieger, R., Michaelis, A., and Green, M. M.

Published
1991
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23. USF2 inhibits the transcriptional activity of Smurf1 and Smurf2 to promote breast cancer tumorigenesis

Author

Zhiqiang Peng, Mengge Du, Ping Xie, Yujiao Chen, and Yawen Tan

Subjects
Transcriptional Activation, 0301 basic medicine, Carcinogenesis, Ubiquitin-Protein Ligases, USF2, Breast Neoplasms, SMAD, medicine.disease_cause, Upstream Stimulatory Factor, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, Cell Line, Tumor, medicine, Humans, Transcription factor, Messenger RNA, biology, Cell Biology, Cell biology, Gene Expression Regulation, Neoplastic, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Upstream Stimulatory Factors, Female, Transforming growth factor
Abstract

Smurf1 (Smad ubiquitylation regulatory factor 1) and Smurf2 are negative regulators of the TGF-β (transforming growth factor-β) pathway. The protein stability and ubiquitin E3 activity regulation of Smurfs have been well studied. However, the mechanism of Smurfs expression at the transcriptional level remains uncharacterized. Here, we reported that USF2 (upstream stimulatory factor 2), a basic helix-loop-helix-leucine-zip transcription factor, is necessary for the transcriptional activity of Smurf1 and Smurf2. The 5'-flanking sequences of the Smurfs gene have more than one E-box motifs, and USF2 bounds the Smurfs promoter in vitro and in vivo. Over-expression USF2 inhibited the transcriptional activity of the Smurfs, and Smurfs mRNA was markedly decreased. Therefore, the activity of TGF-β was distinctly enhanced. Furthermore, in human breast cancers, USF2 was abnormally high expressed and correlated with cancer progression. USF2 was specifically inversely correlated with Smurfs in Luminal A subtype breast cancer patients. These findings suggest the mechanism regulation of Smurfs transcriptional activity, and shed new light on the cancer-promoting role of USF2.

Published
2019

24. Increased SUMOylation of TCF21 improves its stability and function in human endometriotic stromal cells

Author

Qing Xue, Cheng Zeng, Pei-Li Wu, and Jingwen Zhu

Subjects
0301 basic medicine, Stromal cell, Immunoprecipitation, USF2, Endometriosis, SUMO protein, Estrogen receptor, Biology, Upstream Stimulatory Factor, Endometrium, 03 medical and health sciences, 0302 clinical medicine, Basic Helix-Loop-Helix Transcription Factors, Humans, Transcription factor, Chemistry, Sumoylation, Obstetrics and Gynecology, Promoter, Cell Biology, General Medicine, Cell biology, 030104 developmental biology, Reproductive Medicine, 030220 oncology & carcinogenesis, Female, Stromal Cells, Function (biology)
Abstract

Endometriosis is an estrogen-dependent disease. Our previous study demonstrated that elevated levels of transcription factor 21 (TCF21) in endometriotic tissues enhanced steroidogenic factor-1 (SF-1) and estrogen receptor β (ERβ) expression by forming a heterodimer with upstream stimulatory factor 2 (USF2), allowing these TCF21/USF2 complexes to bind to the promoters of SF-1 and ERβ. Furthermore, TCF21 contributed to the increased proliferation of endometriotic stromal cells (ESCs), suggesting that TCF21 may play a vital role in the pathogenesis of endometriosis. SUMOylation is a posttranslational modification that has emerged as a crucial molecular regulatory mechanism. However, the mechanism regulating TCF21 SUMOylation in endometriosis is incompletely characterized. Thus, this study aimed to explore the effect of TCF21 SUMOylation on its expression and regulation in ovarian endometriosis. We found that the levels of SUMOylated TCF21 were increased in endometriotic tissues and stromal cells compared with eutopic endometrial tissues and stromal cells and enhanced by estrogen. Treatment with the SUMOylation inhibitor ginkgolic acid and the results of a protein half-life assay demonstrated that SUMOylation can stabilize the TCF21 protein. A coimmunoprecipitation assay showed that SUMOylation probably increased its interaction with USF2. Further analyses elucidated that SUMOylation of TCF21 significantly increased the binding activity of USF2 to the SF-1 and ERβ promoters. Moreover, the SUMOylation motifs in TCF21 affected the proliferation ability of ESCs. The results of this study suggest that SUMOylation plays a critical role in mediating the high expression of TCF21 in ESCs and may participate in the development of endometriosis.

Published
2021

25. USF2 reduces BMP3 expression via transcriptional activation of miR-34a, thus promoting osteogenic differentiation of BMSCs

Author

Xu-Hui Zhao, Li-Qiang Dong, Yu-Liang Huang, Lian-Guo Wu, Han-Bing Zeng, and Chao Xu

Subjects
Transcriptional Activation, Endocrinology, Diabetes and Metabolism, USF2, Bone Morphogenetic Protein 3, Bone morphogenetic protein 3, Upstream Stimulatory Factor, Endocrinology, stomatognathic system, Downregulation and upregulation, Western blot, Osteogenesis, medicine, Humans, Orthopedics and Sports Medicine, Cells, Cultured, CHIP assay, Reporter gene, biology, medicine.diagnostic_test, Chemistry, Mesenchymal stem cell, Cell Differentiation, General Medicine, Cell biology, MicroRNAs, biology.protein, Upstream Stimulatory Factors
Abstract

Osteoporosis is the most susceptible disease for people over 60. The main cause of osteoporosis is the decreased osteogenic differentiation of mesenchymal stem cells (MSCs). Here we showed that upstream stimulatory factor 2 (USF2)/microRNA-34a (miR-34a)/bone morphogenetic protein 3 (BMP3) axis regulated osteogenic differentiation of BMSCs. USF2 and miR-34a expression were examined using qPCR. Protein levels of BMP3 and osteogenic markers expression were evaluated using both western blot and qPCR. Activity of ALP was determined by ALP assay kit. Mineralization capacity of hBMSCs was assessed using ARS. Besides, CHIP assay was employed to verify whether USF2 could bind to miR-34a promoter. Finally, RIP assay and dual-luciferase reporter assay were employed to verify whether miR-34a directly bound to BMP3. Our results suggested that miR-34a was upregulated during osteogenic differentiation of BMSCs, and miR-34a overexpression could enhance osteogenic differentiation of BMSCs. USF2 could positively regulate miR-34a expression by interacting with its promoter. USF2 overexpression enhanced osteogenic differentiation of BMSCs, while miR-34a inhibition reversed the effect. Besides, BMP3 was the target of miR-34a. MiR-34a overexpression enhanced osteogenic differentiation of BMSCs, which was abolished by BMP3 overexpression. Taken together, USF2 enhanced osteogenic differentiation of BMSCs via downregulating BMP3 by interacting with miR-34a promoter.

Published
2021

26. Tgf-β1 transcriptionally promotes 90K expression: possible implications for cancer progression

Author

Marco Marchisio, Sara Pagotto, Laura De Lellis, Nicola Tinari, Paola Lanuti, Alessandro Cama, Michele De Tursi, Pietro Di Marino, Cesidio Giuliani, Angelo Veronese, Clara Natoli, Antonino Grassadonia, Maurizia D'Egidio, Davide Brocco, Vincenzo Graziano, Patrizia Vici, Graziano, Vincenzo [0000-0001-7656-824X], Pagotto, Sara [0000-0003-2457-6648], Veronese, Angelo [0000-0002-1451-1392], and Apollo - University of Cambridge Repository

Subjects
0301 basic medicine, Cancer Research, 631/337/572/2102, Transcriptional regulatory elements, Immunology, Response element, USF2, USF1, 32 Biomedical and Clinical Sciences, Major histocompatibility complex, Upstream Stimulatory Factor, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, MHC class I, Genetics, 2.1 Biological and endogenous factors, RC254-282, Cancer, 2 Aetiology, biology, QH573-671, MHC Class I Gene, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Growth factor signalling, Cell Biology, Cell biology, 3204 Immunology, 030104 developmental biology, 030220 oncology & carcinogenesis, FOS: Biological sciences, biology.protein, 631/80/86/2368, Cytology, Transforming growth factor
Abstract

The 90K protein, also known as Mac-2 BP or LGALS3BP, can activate the immune response in part by increasing major histocompatibility (MHC) class I levels. In studies on a non-immune cell model, the rat FRTL-5 cell line, we observed that transforming growth factor (TGF)-β1, like γ-interferon (IFN), increased 90K levels, despite its immunosuppressive functions and the ability to decrease MHC class I. To explain this paradoxical result, we investigated the mechanisms involved in the TGF-β1 regulation of 90K expression with the aim to demonstrate that TGF-β1 utilizes different molecular pathways to regulate the two genes. We found that TGF-β1 was able to increase the binding of Upstream Stimulatory Factors, USF1 and USF2, to an E-box element, CANNTG, at −1926 to −1921 bp, upstream of the interferon response element (IRE) in the 90K promoter. Thyrotropin (TSH) suppressed constitutive and γ-IFN-induced 90K expression by decreasing USF binding to the E-box. TGF-β1 was able to overcome TSH suppression at the transcriptional level by increasing USF binding to the E-box. We suggest that the ability of TGF-β1 to increase 90K did not result in an increase in MHC class I because of a separate suppressive action of TGF-β1 directly on the MHC class I gene. We propose that the increased levels of 90K may play a role, rather than in immune response, in the context of the TGF-β1-induced changing of the cellular microenvironment that predisposes to cell motility and cancer progression. Consistently, analyzing the publicly available cancer patient data sets cBioPortal, we found that 90K expression directly correlated with TGF-β1 and USFs and that high levels of 90K were significantly associated with increased mortality in patients affected by different types of cancer.

Published
2020

27. Loss of USF2 promotes proliferation, migration and mitophagy in a redox-dependent manner

Author

Fawzi Khoder-Agha, IIkka Miinalainen, Thomas Kietzmann, Sakari Kellokumpu, Daniela Mennerich, Elitsa Y. Dimova, and Tabughang Franklin Chi

Subjects
0301 basic medicine, Clinical Biochemistry, USF2, Proliferation, Biochemistry, Energy homeostasis, Upstream Stimulatory Factor, law.invention, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, law, Mitophagy, medicine, Promoter Regions, Genetic, Protein kinase B, Transcription factor, lcsh:QH301-705.5, Migration, Cell Proliferation, lcsh:R5-920, Chemistry, Organic Chemistry, Upstream stimulatory factor 2 (USF2), Compromised mitochondria, medicine.disease, Cell biology, 030104 developmental biology, lcsh:Biology (General), Gene Expression Regulation, Suppressor, lcsh:Medicine (General), Oxidation-Reduction, 030217 neurology & neurosurgery, Research Paper
Abstract

The upstream stimulatory factor 2 (USF2) is a transcription factor implicated in several cellular processes and among them, tumor development seems to stand out. However, the data with respect to the role of USF2 in tumor development are conflicting suggesting that it acts either as tumor promoter or suppressor. Here we show that absence of USF2 promotes proliferation and migration. Thereby, we reveal a previously unknown function of USF2 in mitochondrial homeostasis. Mechanistically, we demonstrate that deficiency of USF2 promotes survival by inducing mitophagy in a ROS-sensitive manner by activating both ERK1/2 and AKT. Altogether, this study supports USF2′s function as tumor suppressor and highlights its novel role for mitochondrial function and energy homeostasis thereby linking USF2 to conditions such as insulin resistance, type-2 diabetes mellitus, and the metabolic syndrome.

Published
2020

28. Phosphorylation of E‐box binding USF‐1 by PI3K/AKT enhances its transcriptional activation of the WBP2 oncogene in breast cancer cells

Author

Qing Hao Miow, Alisha Ramos, Qing Song Lin, Thomas C. Putti, Yoon Pin Lim, and Xu Liang

Subjects
0301 basic medicine, Chemistry, Wnt signaling pathway, Estrogen receptor, medicine.disease_cause, Biochemistry, Upstream Stimulatory Factor, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Genetics, medicine, Carcinogenesis, Molecular Biology, Transcription factor, Protein kinase B, Chromatin immunoprecipitation, PI3K/AKT/mTOR pathway, Biotechnology
Abstract

WW domain binding protein 2 (WBP2), a transcriptional coactivator, plays a vital role in breast tumorigenesis. It positively regulates estrogen receptor, Hippo, and Wnt pathways, which subsequently enhance the transcription of downstream target genes contributing to cancer. Understanding the regulation of the expression and activity of WBP2 oncoprotein has implication in cancer therapy. We have previously reported that WBP2 is regulated at the post-translational and post-transcriptional levels. However, its regulation at the transcriptional level is not known. In this study, the minimal promoter region of WBP2 that is critical for its transcription was identified. The E-box motif in the WBP2 promoter was demonstrated to be essential for its transcription. The E-box binding protein upstream stimulatory factor 1 (USF-1) was discovered to be a key transcription factor for WBP2 by yeast one-hybrid analysis and was validated through reporter and chromatin immunoprecipitation assays and tandem mass spectrometry, which also suggested that USF-1 acts by regulating a network of genes, in addition to WBP2, associated with cell movement, proliferation, cell-cycle, and survival cellular processes. USF-1 is overexpressed in majority of the breast cancer cell lines and tissues tested, and has profound effects on cancer cell proliferation. USF-1-mediated transcription of WBP2 was demonstrated to be inducible by insulin, which led to AKT-mediated phosphorylation of USF-1 that modulated its ability to bind to the WBP2 promoter and activate its transcription. This study sheds new light onto the regulation of the WBP2 oncogene at the transcriptional level by a novel oncogenic transcription factor, USF-1. USF-1 is a potential drug target for treatment of WBP2-positive breast cancer.-Ramos, A., Miow, Q. H., Liang, X., Lin, Q. S., Putti, T. C., Lim, Y. P. Phosphorylation of E-box binding USF-1 by PI3K/AKT enhances its transcriptional activation of the WBP2 oncogene in breast cancer cells.

Published
2018

29. Transcription factor 21 regulates expression of ERβ and SF-1 via upstream stimulatory factor-2 in endometriotic tissues

Author

Qing Xue, Pei Li Wu, Zhao Tong Dong, Xin Li, Yan Zhou, Serdar E. Bulun, Cheng Zeng, and Ying Fang Zhou

Subjects
Adult, 0301 basic medicine, USF2, Biophysics, Mice, Nude, Steroidogenic Factor 1, Biochemistry, Upstream Stimulatory Factor, E-Box Elements, Mice, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Gene expression, Basic Helix-Loop-Helix Transcription Factors, Genetics, Transcriptional regulation, Animals, Estrogen Receptor beta, Humans, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Cells, Cultured, Estrogen receptor beta, Cell Proliferation, Gene knockdown, Chemistry, Promoter, Cell biology, 030104 developmental biology, Gene Expression Regulation, 030220 oncology & carcinogenesis, Upstream Stimulatory Factors, Female, Stromal Cells, Endometritis
Abstract

Steroidogenic factor-1 (SF-1, encoded by NR5A1) and estrogen receptor beta (ERβ, encoded by ESR2), which are highly expressed in endometriotic stromal cells (ESCs), contribute to the pathogenesis of endometriosis, but the regulation mechanism remains largely unknown. Transcription factor 21 (TCF21) belongs to the helix-loop-helix (bHLH) family characterized by regulating gene expression via binding to E-box element. Here, we attempted to determine the molecular mechanism of TCF21 on SF-1 and ERβ expression in endometriosis. We found that TCF21 expression in ESCs was higher than that in endometrial stromal cells (EMs), and positively correlated with SF-1 and ERβ expression in ESCs. Since the importance of E-box element for NR5A1 promoter activity has been previously reported, we performed site-mutation and luciferase assay, revealing that the E-box sequence in the ESR2 promoter is also a critical element modulating ERβ expression. Upstream stimulatory factor 2 (USF2) is another bHLH factor implicated in transcriptional regulation. Further analyses elucidated that it is not TCF21, but USF2 exhibited higher binding affinities in ESCs to NR5A1 and ESR2 promoters than in EMs. Additionally, TCF21 knockdown significantly decreased the binding activities of USF2 to NR5A1 and ESR2 promoters via disruption of the TCF21-USF2 complex. Meanwhile, manipulating TCF21 expression significantly affected MMP9 and cyclinD1 expression, as wells as proliferation and invasion of ESCs. Moreover, TCF21 depletion in endometriotic xenografts reduced SF-1 and ERβ expression, abrogating ectopic lesion growth in mice. Cumulatively, a critical role of TCF21 in the pathogenesis of endometriosis is demonstrated, suggesting a potential druggable target for future therapy.

Published
2018

30. Interleukin-like EMT inducer (ILEI) promotes melanoma invasiveness and is transcriptionally up-regulated by upstream stimulatory factor-1 (USF-1)

Author

Bidyut K. Mohanty, Breege V. Howley, Buckley J. McCall, Toros Dincman, Annamarie C. Dalton, Ken Noguchi, and Philip H. Howe

Subjects
Transcriptional Activation, 0301 basic medicine, Epithelial-Mesenchymal Transition, mRNA, Cell, phenotype switching, Biochemistry, Upstream Stimulatory Factor, Cell Line, Mice, 03 medical and health sciences, Downregulation and upregulation, Cell Line, Tumor, melanoma, cytokine, medicine, Transcriptional regulation, Animals, Humans, Gene Regulation, Neoplasm Invasiveness, Epithelial–mesenchymal transition, Molecular Biology, Transcription factor, transcription factor, FAM3C, Cells, Cultured, USF-1, Gene knockdown, ILEI, Chemistry, Melanoma, Cell Biology, medicine.disease, Neoplasm Proteins, Up-Regulation, 3. Good health, Gene Expression Regulation, Neoplastic, epithelial-mesenchymal transition (EMT), 030104 developmental biology, medicine.anatomical_structure, interleukin-like EMT inducer, Cancer research, Cytokines, Upstream Stimulatory Factors
Abstract

Interleukin-like EMT inducer (ILEI, FAM3C) is a secreted factor that contributes to the epithelial-to-mesenchymal transition (EMT), a cell-biological process that confers metastatic properties to a tumor cell. However, very little is known about how ILEI is regulated. Here we demonstrate that ILEI is an in vivo regulator of melanoma invasiveness and is transcriptionally up-regulated by the upstream stimulatory factor-1 (USF-1), an E-box–binding, basic-helix-loop-helix family transcription factor. shRNA-mediated knockdown of ILEI in melanoma cell lines attenuated lung colonization but not primary tumor formation. We also identified the mechanism underlying ILEI transcriptional regulation, which was through a direct interaction of USF-1 with the ILEI promoter. Of note, stimulation of endogenous USF-1 by UV-mediated activation increased ILEI expression, whereas shRNA-mediated USF-1 knockdown decreased ILEI gene transcription. Finally, we report that knocking down USF-1 decreases tumor cell migration. In summary, our work reveals that ILEI contributes to melanoma cell invasiveness in vivo without affecting primary tumor growth and is transcriptionally up-regulated by USF-1.

Published
2018

31. Hepatocyte nuclear factor 4α regulates the expression of the murine pyruvate carboxylase gene through the HNF4-specific binding motif in its proximal promoter.

Author

Chavalit, Tanit, Rojvirat, Pinnara, Muangsawat, Sureeporn, and Jitrapakdee, Sarawut

Abstract

Abstract: Pyruvate carboxylase (PC) is the first regulatory enzyme of gluconeogenesis. Here we report that the proximal promoter of the murine PC gene contains three binding sites for hepatocyte nuclear factor 4α (HNF4α). These sites include the classical direct repeat 1 (DR1) (−386/−374), non-perfect DR1 (−118/−106) and HNF4α-specific binding motif (H4-SBM) (−26/−14). Under basal conditions, mutation of the non-perfect DR1 decreased promoter activity by 50%, whereas mutation of neither the DR1 nor the H4-SBM had any effect. In marked contrast, only mutation of the H4-SBM decreased HNF4α-transactivation of the promoter activity by 65%. EMSA revealed that HNF4α binds to the DR1site and H4-SBM with similar affinity while it binds poorly to the non-perfect DR1. Interestingly, this non-perfect DR1 also coincides with two E-boxes. Mutation of the non-perfect DR1 together with the nearby E-box reduced USF1- but not USF2-transactivation of promoter activity, suggesting that USF1 partly contributes to the basal activity of the promoter. Substitution of the H4-SBM with the DR1 marginally reduced the basal promoter activity but did not eliminate HNF4α-transactivation, suggesting that HNF4α can exert its effect via DR1 within this promoter context. ChIP-assay confirmed that HNF4α is associated with the H4-SBM. Suppression of HNF4α expression in AML12 cells down-regulated PC mRNA and PC protein by 60% and 50%, respectively, confirming that PC is a target of HNF4α. We also propose a model for differential regulation of P1 promoter of PC gene in adipose tissue and liver. [Copyright &y& Elsevier]

Published
2013
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32. Transcriptional regulation of lipogenesis and its contribution to hepatosteatosis.

Author

Wang, Yuhui and Sul, Hei Sook

Subjects
*LIPID synthesis, *INSULIN therapy, *LIVER diseases, *THERAPEUTICS, *FATTY liver, *TREATMENT of cirrhosis of the liver
Abstract

"Agents that can block lipogenesis or molecules involved in the activation of lipogenic genes might be attractive candidates as therapeutics for the prevention and treatment of hepatosteatosis." [ABSTRACT FROM AUTHOR]

Published
2013
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33. Metoprolol represses PGC1α-mediated carnitine palmitoyltransferase-1B expression in the diabetic heart

Author

Sharma, Vijay, Dhillon, Pavan, Parsons, Hannah, Allard, Michael F., and McNeill, John H.

Subjects
*METOPROLOL, *TRANSFERASES, *GENE expression, *HEART failure, *PEOPLE with diabetes, *TRANSCRIPTION factors, *CARDIOMYOPATHIES
Abstract

Abstract: We have previously shown that metoprolol decreases carnitine palmitoyltransferase-1 (CPT-1) activity, a mechanism which may partly explain its beneficial effects in heart failure. It is possible that this effect occurs as a result of repression of cardiac CPT-1B expression. CPT-1B is induced by the transcription factors peroxisome proliferator activated receptor-α (PPAR-α) and PPAR-γ-coactivator 1α (PGC1α) and repressed by upstream stimulatory factor-2 (USF-2). We therefore hypothesized that metoprolol represses CPT-1B by increasing USF-2-mediated repression of PGC1α. Male Wistar Rats were divided into 4 groups: control, control treated with metoprolol for 5 weeks, diabetic and diabetic treated with metoprolol for 5 weeks. After termination, the expression of CPT-1 isoforms, PPAR-α, PGC1α USF-1 and USF-2, as well as downstream targets were measured. Binding of PPAR-α, PGC1α and USF-2 to PGC1α was measured using coimmunoprecipitation. The occupation of PPAR-α and MEF-2A consensus sites in the CPT-1B promoter was measured using chromatin immunoprecipitation assays. Chronic metoprolol treatment decreased the expression of CPT-1B in diabetic hearts. The expression of USF-2 was increased by metoprolol in both control and diabetic hearts, but the association of USF-2 with PGC1α was increased by metoprolol only in diabetic hearts. Metoprolol prevented the increase in PGC1α occupation of the CPT-1B promoter region observed in the diabetic heart without affecting PPAR-α occupation. Metoprolol decreases CPT-1B expression by decreasing PGC1α-mediated coactivation of PPAR-α and MEF-2A. This is associated with increased PGC1α/ USF-2 binding, suggesting that USF-2 mediates the metoprolol-induced repression of PGC1α. [Copyright &y& Elsevier]

Published
2009
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34. Glucose increases hepatic lipase expression in HepG2 liver cells through upregulation of upstream stimulatory factors 1 and 2.

Author

Deursen, D., Jansen, H., and Verhoeven, A.

Abstract

Elevated hepatic lipase ( HL, also known as LIPC) expression is a key factor in the development of the atherogenic lipid profile in type 2 diabetes and insulin resistance. Recently, genetic screens revealed a possible association of type 2 diabetes and familial combined hyperlipidaemia with the USF1 gene. Therefore, we investigated the role of upstream stimulatory factors (USFs) in the regulation of HL. Levels of USF1, USF2 and HL were measured in HepG2 cells cultured in normal- or high-glucose medium (4.5 and 22.5 mmol/l, respectively) and in livers of streptozotocin-treated rats. Nuclear extracts of cells cultured in high glucose contained 2.5 ± 0.5-fold more USF1 and 1.4 ± 0.2-fold more USF2 protein than cells cultured in normal glucose (mean ± SD, n = 3). This coincided with higher DNA binding of nuclear proteins to the USF consensus DNA binding site. Secretion of HL (2.9 ± 0.5-fold), abundance of HL mRNA (1.5 ± 0.2-fold) and HL (–685/+13) promoter activity (1.8 ± 0.3-fold) increased in parallel. In chromatin immunoprecipitation assays, the proximal HL promoter region was immunoprecipitated with anti-USF1 and anti-USF2 antibodies. Co-transfection with USF1 or USF2 cDNA stimulated HL promoter activity 6- to 16-fold. USF and glucose responsiveness were significantly reduced by removal of the −310E-box from the HL promoter. Silencing of the USF1 gene by RNA interference reduced glucose responsiveness of the HL (−685/+13) promoter region by 50%. The hyperglycaemia in streptozotocin-treated rats was associated with similar increases in USF abundance in rat liver nuclei, but not with increased binding of USF to the rat Hl promoter region. Glucose increases HL expression in HepG2 cells via elevation of USF1 and USF2. This mechanism may contribute to the development of the dyslipidaemia that is typical of type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published
2008
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35. Cooperative activation of lipocalin-type prostaglandin D synthase gene expression by activator protein-2β in proximal promoter and upstream stimulatory factor 1 within intron 4 in human brain-derived TE671 cells

Author

Fujimori, Ko and Urade, Yoshihiro

Subjects
*GENE expression, *GENETIC regulation, *ADENOSINE triphosphatase gene expression, *BACTERIOPHAGE mu gene expression
Abstract

Abstract: We investigated the activation mechanism of gene expression of lipocalin-type prostaglandin D synthase (L-PGDS) in human brain-derived TE671 cells. Reporter analyses of constructs carrying various lengths of the promoter region and intron 1 to 6, or 3′-untranslated region of the human L-PGDS gene demonstrated that one atypical E-box (aE-box) at +2569 in intron 4 was critical for transactivation of the gene. The aE-box inside the intron 4 functioned as an enhancer element in both directions and in a cell-type specific manner in TE671 cells. Yeast one-hybrid screening revealed that upstream stimulatory factor (USF) 1 bound to the aE-box. Expression of exogenous USF1 induced the endogenous L-PGDS expression in TE671 cells, whereas administration of USF1 siRNA suppressed L-PGDS expression. Binding of USF1 to the aE-box was confirmed by performing electrophoretic mobility shift assay and chromatin immunoprecipitation assay. Furthermore, USF1-mediated transcriptional activation was dependent upon activator protein (AP)-2β binding to the AP-2 element at position −98 in the proximal promoter region of human L-PGDS gene. These results indicate that L-PGDS gene expression in TE671 cells was activated by USF1 through the aE-box within intron 4 and cooperatively by AP-2β in the promoter in a cell-type-specific manner. [Copyright &y& Elsevier]

Published
2007
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36. Regulation of Transforming Growth Factor β in Diabetic Nephropathy: Implications for Treatment.

Author

Zhu, Yanqing, Usui, Hitomi Kataoka, and Sharma, Kumar

Subjects
TRANSFORMING growth factors-beta, DIABETIC nephropathies, PROTEIN kinase C, REACTIVE oxygen species, THROMBOSPONDINS, MACROPHAGES, STIMULANTS, GENETIC regulation, THERAPEUTICS
Abstract

Summary: The recognition that the drivers of matrix accumulation is an appropriate therapeutic target for diabetic nephropathy is now accepted by the nephrology and pharmaceutical communities. Interventions focused around transforming growth factor-β (TGF-β) likely will be an important area of clinical investigation in the near future. Understanding the various pathways involved in stimulating TGF-β in the diabetic kidney is of paramount importance in devising strategies to combat the development and progression of diabetic nephropathy. In this review we highlight the major pathways involved in stimulating TGF-β production by increased glucose levels and discuss the therapeutic implications thereof. [ABSTRACT FROM AUTHOR]

Published
2007
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37. Identification of an E-box motif as a transcriptional repressor element in the proximal promoter region of the GCLC gene in rat lung epithelial L2 cells

Author

Cheng, Lin-Ling, Li, Bing, Luo, Jian-Dong, Tu, Hong-Bin, Liu, Qi-Cai, and Ran, Pixin

Subjects
*GLUTATHIONE, *ENZYMES, *RESPIRATORY diseases, *GENETIC mutation
Abstract

Abstract: Glutathione (GSH) is a critical antioxidant for protecting the airway epithelium from oxidant injury and its levels are mainly controlled by glutamate-cysteine ligase (GCL), which is the rate-limiting enzyme in GSH synthesis. A full understanding of the gene regulation mechanism of this important enzyme may disclose the role it plays in respiratory diseases. GCL is made up of two differentially regulated subunits, a catalytic or heavy subunit (GCLC) and a modifier or light subunit (GCLM). Many studies in this field led to the findings of important positive regulatory regions of the GCLC promoter. For a detailed analysis of this gene regulation in the respiratory system, we cloned a 1.76-kb 5′-flanking region of the rat GCLC gene, inserted into a luciferase reporter vector. Exonuclease III was used to cut the 5′-flanking region of the rat GCLC gene unidirectionally into deletion mutants of different lengths. Sequential deletion analysis revealed that regions from −403 to −111 and from −705 to −613 are involved in positive regulation and the region from −745 to −705 is involved in negative regulation of the GCL gene in rat lung epithelial L2 cells. Specific proteins binding to these regions were confirmed by electrophoretic mobility-shift assays (EMSAs) and antibody supershift assays. An E-box motif was found in the negative regulatory region −745 to −705. Site-directed mutagenesis proved that the functional element in this negative regulatory region was a putative E-box element. EMSA and supershift assays showed that USF1 and USF2 can specifically bind to the E-box element. Overexpression of USFs in L2 cells led to a decreased activity of the GCLC promoter. Western blotting demonstrated that the expression of GCLC protein was decreased in the retroviral USFs-expressing cells than in nontransfected (no DNA added) cells, suggesting that USF binding to the E-box at −729/−724 serves to trans-repress GCLC gene expression. These findings indicate that the E-box is an important transcriptional suppressor element in the GCLC promoter in rat lung epithelial L2 cells. Inhibition of interaction between the E-box and the USF may provide an effective means of ameliorating oxidant injury of the lung. [Copyright &y& Elsevier]

Published
2005
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38. Mutations including the promoter region of myocilin/TIGR gene.

Author

Saura, Maria, Cabana, Montse, Ayuso, Carmen, and Valverde, Diana

Subjects
*GLAUCOMA, *EYE diseases, *TRANSCRIPTION factors, *PROTEINS, *HUMAN genetics, *GENETICS, *HUMAN heredity, *HUMAN biology
Abstract

Mutations in the MYOC/TIGR gene are responsible for autosomal dominant primary open angle glaucoma (POAG). Almost all mutations responsible for POAG have been detected in the coding region (in particular at exon 3). By using the techniques of PCR, SSCP, automated sequencing and restriction analysis, we have studied 79 patients suffering from glaucoma. We have found five patients with sequence variants in the consensus region of the promoter. These sequence variants might be involved in the altered association between the consensus region and the corresponding transcription factor. This possibility might be favouring the association of other transcription factors, which would operate as activators or inhibitors of the transcription, altering the MYOC/TIGR expression.European Journal of Human Genetics (2005) 13, 384-387. doi:10.1038/sj.ejhg.5201299 Published online 13 October 2004 [ABSTRACT FROM AUTHOR]

Published
2005
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39. Characterization of the promoter of 1A6/DRIM, a novel cancer-related gene and identification of its transcriptional activator

Author

Xing, Xiaoyan, Du, Xiaojuan, Lu, Zheming, Ning, Tao, Su, Xiulan, and Ke, Yang

Subjects
*IN situ hybridization, *DNA polymerases, *POLYMERASE chain reaction
Abstract

Abstract: 1A6/DRIM (Down-regulated in Metastasis) has been reported to express at a high level in the gastric cancer tissues and the premalignant lesions implicating the involvement of 1A6/DRIM in cell transformation. Although the information regarding the putative functions and distribution of the 1A6/DRIM in different tissues and cell lines has been increasing recently, its promoter and promoter-regulating factors remain unknown. In this study, the transcription initiation site of 1A6/DRIM was confirmed to be located at 147 bp upstream of the ATG codon using the primer extension analysis. The minimal promoter region of the 1A6/DRIM is located between −47 and +42 of the transcription initiation site measured by luciferase reporter assays using a set of deletion constructs. In addition, an E-box is shown to be an essential element for transcriptional regulation of 1A6/DRIM demonstrated by luciferase assay with different deletion and mutation constructs. Finally, a transcription factor, upstream stimulatory factor 2 (USF2) was found to be an activator of the 1A6/DRIM through binding to the E-box demonstrated by luciferase reporter assay, electrophoretic mobility shift assay, and chromatin immunoprecipitation (ChIP) assay. The structural analysis of the 1A6/DRIM promoter and the identification of its potential regulatory effecter may help us to understand its biological functions in regulating cancer development. [Copyright &y& Elsevier]

Published
2005
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40. The complicated dialogue between Helicobacter pylori and p53

Author

Jing-Yuan Fang and Zhi-Hang Tao

Subjects
biology, business.industry, Gastroenterology, Cancer research, USF1, biology.protein, Medicine, Helicobacter pylori, business, Gastric carcinogenesis, biology.organism_classification, Upstream Stimulatory Factor
Abstract

We recently read the interesting paper published in GUT elucidating the role of upstream stimulatory factor 1 (USF1) in Helicobacter pylori (Hp )-induced p53 degradation.1 The work greatly broadens our knowledge of the interplay between Hp and p53 during gastric carcinogenesis. Here we propose some additional exploration, if incorporated in study design, can further deepen our understanding. The significance of USF1 in gastric carcinogenesis should be acknowledged as the study showed that loss of USF1, on its own, exacerbated the severity of …

Published
2020

41. The rat enhancer of split- and hairy-related protein-2 gene: hepatic expression, genomic structure, and promoter analysis

Author

Hirano, Satoko, Yamada, Kazuya, Kawata, Hiroko, Shou, Zhangfei, Mizutani, Tetsuya, Shigematsu, Yousuke, Mayumi, Mitsufumi, and Miyamoto, Kaoru

Subjects
*PROTEINS, *TRANSCRIPTION factors, *MESSENGER RNA, *HEPATOCELLULAR carcinoma
Abstract

The rat enhancer of split- and hairy-related protein-2 (SHARP-2) is a basic helix-loop-helix transcription factor. The hepatic expression of SHARP-2 mRNA was investigated under various conditions. The level was decreased in the regenerating rat liver and malignant hepatoma cells. In contrast, the expression of SHARP-2 mRNA was induced in rat livers by feeding a high-carbohydrate diet. To analyze the molecular mechanism involved in the regulation of the rat SHARP-2 gene expression, the gene was cloned. It was approximately 6-kb in length and consists of five exons and four introns. To investigate the transcriptional regulatory region of this gene, SHARP-2/firefly luciferase reporter plasmids were transfected into hepatoma cells. A functional analysis of 5′-deletion constructs revealed that two E box sequences between –160 and –144 are mainly responsible for promoter activity. Although upstream stimulatory factors (USFs) bound to the element in vitro, USF2 failed to stimulate promoter activity from the element using the co-transfection experiment. Therefore, other E box-binding transcription factors differing from USF proteins or USF-associated proteins are necessary for transcriptional stimulation of the rat SHARP-2 gene. [Copyright &y& Elsevier]

Published
2004
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42. Variant forms of upstream stimulatory factors (USFs) control the promoter activity of hTERT, the human gene encoding the catalytic subunit of telomerase

Author

Yago, Masako, Ohki, Rieko, Hatakeyama, Shinji, Fujita, Toshiro, and Ishikawa, Fuyuki

Subjects
*TELOMERASE, *REVERSE transcriptase, *LYMPHOCYTES
Abstract

It is known that Myc regulates the expression of TERT, the telomerase catalytic subunit gene, by binding to E box. Here we show that another E box-binding protein, upstream stimulatory factor (USF), also regulates TERT expression. Specifically, the N-terminally truncated form of USF2 is present in telomerase-negative/resting human lymphocytes, but not in telomerase-positive/phytohemagglutinin-activated lymphocytes. In electrophoretic mobility shift assay, both full-length and truncated USF2s bound to the TERT E box. In a transient expression assay, the truncated USF had a dominant-negative effect on both exogenous full-length USF and endogenous positive regulators for activating TERT expression. These results suggest that the differential abundance of truncated USF2 may regulate telomerase activity during lymphocyte activation. [Copyright &y& Elsevier]

Published
2002
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43. Hepatitis C Virus Induces the Ubiquitin-Editing Enzyme A20 via Depletion of the Transcription Factor Upstream Stimulatory Factor 1 To Support Its Replication

Author

Ja Yeon Kim, Stephanie T. Chan, Jing-hsiung James Ou, and Jiyoung Lee

Subjects
hcv ires, Hepacivirus, Virus Replication, Microbiology, Upstream Stimulatory Factor, Host-Microbe Biology, Cell Line, 03 medical and health sciences, immune system diseases, hemic and lymphatic diseases, Virology, medicine, Humans, a20 ubiquitin enzyme, Gene silencing, Promoter Regions, Genetic, Transcription factor, Tumor Necrosis Factor alpha-Induced Protein 3, 030304 developmental biology, 0303 health sciences, Host Microbial Interactions, 030306 microbiology, Chemistry, Ubiquitination, virus diseases, usf-1 transcription factor, hepatitis c virus, Hepatitis C, QR1-502, digestive system diseases, 3. Good health, Cell biology, Internal ribosome entry site, Gene Expression Regulation, Proteasome, Proteasome inhibitor, Upstream Stimulatory Factors, Signal transduction, Chromatin immunoprecipitation, Research Article, Signal Transduction, medicine.drug
Abstract

Hepatitis C virus establishes chronic infection in approximately 85% of the patients whom it infects. However, the mechanism of how HCV evades host immunity to establish persistence is unclear. In this report, we demonstrate that HCV could induce the expression of the ubiquitin-editing enzyme A20, an important negative regulator of the tumor necrosis factor alpha (TNF-α) and NF-κB signaling pathways. This induction of A20 enhanced HCV replication as it could stimulate the HCV IRES activity to enhance the translation of HCV proteins. The induction of A20 was mediated by the depletion of USF-1, a suppressor of the A20 promoter. Our study thus provides important information for further understanding the interaction between HCV and its host cells., Tumor necrosis factor alpha-induced protein 3 (TNFAIP3), also known as A20, is a ubiquitin-editing enzyme capable of ubiquitination or deubiquitination of its target proteins. In this study, we show that hepatitis C virus (HCV) infection could induce the expression of A20 via the activation of the A20 promoter. The induction of A20 by HCV coincided with the loss of upstream stimulatory factor 1 (USF-1), a transcription factor known to suppress the A20 promoter. The role of USF-1 in the regulation of the A20 promoter in HCV-infected cells was confirmed by the chromatin immunoprecipitation (ChIP) assay, and its depletion was apparently mediated by proteasomes, as USF-1 could be stabilized by the proteasome inhibitor MG132 to suppress the A20 expression. As the overexpression of A20 enhanced the replication of HCV and the silencing of A20 had the opposite effect, A20 is a positive regulator of HCV replication. Our further studies indicated that A20 enhanced the activity of the HCV internal ribosome entry site (IRES). In conclusion, our results demonstrated that HCV could induce the expression of A20 via the depletion of USF-1 to enhance its replication. Our study provided important information for further understanding the interaction between HCV and its host cells.

Published
2019

44. The nuclear fraction of protein kinase CK2 binds to the upstream stimulatory factors (USFs) in the absence of DNA

Author

Thomas Kietzmann, Mathias Montenarh, Sarah Spohrer, Elitsa Y. Dimova, and Claudia Götz

Subjects
0301 basic medicine, animal structures, Protein subunit, USF2, Biology, Upstream Stimulatory Factor, Cell Line, Protein–protein interaction, 03 medical and health sciences, chemistry.chemical_compound, Casein Kinase II, Transcription factor, Cell Nucleus, Kinase, fungi, DNA, Cell Biology, Molecular biology, Cell biology, 030104 developmental biology, chemistry, embryonic structures, Upstream Stimulatory Factors, Phosphorylation, Protein Binding
Abstract

The functions of the upstream stimulatory factors USF1 and USF2 are, like those of other transcription factors, regulated by reversible phosphorylation. Besides many other kinases also protein kinase CK2 phosphorylates USF1 but not USF2. In a yeast-two-hybrid screen, however, the non-catalytic CK2β subunit of CK2 was identified as a binding partner of USF2. This surprising observation prompted us to investigate the CK2/USF interaction in more detail in the present study. By using immunofluorescence analyses as well as co-immunoprecipitations we found that USF1 and USF2 bound to CK2α and CK2β exclusively in the nucleus, though CK2β and to a minor amount CK2α were also present in the cytoplasm. Furthermore, we found that unlike other substrates the phosphorylation of USF1 required the presence of the regulatory CK2β subunit; the catalytic α-subunit of CK2 alone was not able to phosphorylate USF1. Thus, the correct phosphorylation of USF1 is only guaranteed and strictly controlled in particular by nuclear CK2β. Although the data indicated that a nuclear subfraction of CK2 subunits associated with USF proteins, DNA pull down experiments revealed that the CK2 subunits did not co-localize with DNA bound USF proteins indicating that the USF/CK2 interaction has a pre- or post DNA binding function.

Published
2016

45. The basic region/helix-loop-helix/leucine repeat transcription factor USF interferes with Ras transformation.

Author

Aperlo, Christel, Boulukos, Kim E., and Pognonec, Philippe

Subjects
*TRANSCRIPTION factors, *DNA-binding proteins, *MYC oncogenes, *BINDING sites, *RAS oncogenes, *PROTEIN binding
Abstract

Upstream stimulatory factor (USF) is a transcription factor of the basic region/helix-loop-helix/leucine repeat family. It shares the same DNA-binding sequence as the myc oncogene. Based on the three-dimensional structures, its DNA-binding domain is structurally related to that of Max, the partner of Myc. In addition, USF can form heterodimers with a related factor, Fos-interacting protein/upstream stimulatory factor 2 (FIP/USF2), which ahs been shown to directly interact with Fos. In view of the provocative relationship of USF with other factors involved in cell proliferation, we investigated whether USF could also play a role in cellular growth control. In this study, we report that USF is not an oncogene, but interfered with Ras-driven transformation. This inhibitory effect is dependent of USF transactivating domains, but requires its DNA-binding activity. However, the minimal USF DNA-binding domain does not display this inhibitory effect, and even slightly enhances Ras transformation. On the basis of these data, we propose that USF may play an important role in the control of cell growth and proliferation, through both binding to promoter sequences and specific protein/protein interactions. [ABSTRACT FROM AUTHOR]

Published
1996
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46. Role of upstream stimulatory factor 2 in glutamate dehydrogenase gene transcription

Author

Isabel V. Baanante, Jonás I. Silva-Marrero, María C. Salgado, Isidoro Metón, and Carlos Gaspar

Subjects
0301 basic medicine, Transcriptional Activation, Transcription, Genetic, 5' Flanking Region, Molecular biology, USF2, Upstream Stimulatory Factor, E-Box Elements, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Glutamate Dehydrogenase, Transcription (biology), Sparus aurata, Transcriptional regulation, Genetics, Animals, Tissue Distribution, Promoter Regions, Genetic, Molecular Biology, Biologia molecular, Messenger RNA, Base Sequence, Chemistry, Glutamate dehydrogenase, Inanició, Sea Bream, Orada, Cell biology, Diet, Alimentació, 030104 developmental biology, Liver, Starvation, Mutation, Upstream Stimulatory Factors, NAD+ kinase, Chromatin immunoprecipitation, 030217 neurology & neurosurgery, Genètica, Protein Binding
Abstract

Glutamate dehydrogenase (Gdh) plays a central role in ammonia detoxification by catalysing reversible oxidative deamination ofl-glutamate into α-ketoglutarate using NAD+or NADP+as cofactor. To gain insight into transcriptional regulation ofglud, the gene that codes for Gdh, we isolated and characterised the 5′ flanking region ofgludfrom gilthead sea bream (Sparus aurata). In addition, tissue distribution, the effect of starvation as well as short- and long-term refeeding on Gdh mRNA levels in the liver ofS. auratawere also addressed. 5′-Deletion analysis ofgludpromoter in transiently transfected HepG2 cells, electrophoretic mobility shift assays, chromatin immunoprecipitation (ChIP) and site-directed mutagenesis allowed us to identify upstream stimulatory factor 2 (Usf2) as a novel factor involved in the transcriptional regulation ofglud. Analysis of tissue distribution of Gdh and Usf2 mRNA levels by reverse transcriptase-coupled quantitative real-time PCR (RT-qPCR) showed that Gdh is mainly expressed in the liver ofS. aurata, while Usf2 displayed ubiquitous distribution. RT-qPCR and ChIP assays revealed that long-term starvation down-regulated the hepatic expression of Gdh and Usf2 to similar levels and reduced Usf2 binding togludpromoter, while refeeding resulted in a slow but gradual restoration of both Gdh and Usf2 mRNA abundance. Herein, we demonstrate that Usf2 transactivatesS. aurata gludby binding to an E-box located in the proximal region ofgludpromoter. In addition, our findings provide evidence for a new regulatory mechanism involving Usf2 as a key factor in the nutritional regulation ofgludtranscription in the fish liver.

Published
2018

47. Transcriptional activation of Epstein–Barr virus BRLF1 by USF1 and Rta

Author

Chen-Chia Hung, Shih-Tung Liu, Tzu-Hsuan Chang, Wen-Hung Wang, Li-Kwan Chang, Chung-Wen Kuo, and Pey-Jium Chang

Subjects
Gene Expression Regulation, Viral, Transcriptional Activation, Epstein-Barr Virus Infections, Herpesvirus 4, Human, viruses, Molecular Sequence Data, Response element, Biology, medicine.disease_cause, Upstream Stimulatory Factor, Immediate early protein, Immediate-Early Proteins, Plasmid, Transcription (biology), Virology, medicine, Humans, Promoter Regions, Genetic, Binding Sites, Base Sequence, Transfection, biochemical phenomena, metabolism, and nutrition, Epstein–Barr virus, Molecular biology, Lytic cycle, Host-Pathogen Interactions, Trans-Activators, Upstream Stimulatory Factors, Protein Binding
Abstract

During its lytic cycle, Epstein-Barr virus (EBV) expresses Rta, a factor encoded by BRLF1 that activates the transcription of viral lytic genes. We found that upstream stimulating factor (USF) binds to E1, one of the five E boxes located at - 79 in the BRLF1 promoter (Rp), to activate BRLF1 transcription. Furthermore, Rta was shown to interact with USF1 in coimmunoprecipitation and glutathione S-transferase (GST)-pulldown assays, and confocal laser-scanning microscopy further confirmed that these two proteins colocalize in the nucleus. Rta was also found to bind with the E1 sequence in a biotin-labelled E1 probe, but only in the presence of USF1, suggesting that these two proteins likely form a complex on E1. We subsequently constructed p188mSZ, a reporter plasmid that contained the sequence from - 188 to +5 in Rp, within which the Sp1 site and Zta response element were mutated. In EBV-negative Akata cells cotransfected with p188mSZ and plasmids expressing USF1 and Rta, synergistic activation of Rp transcription was observed. However, after mutating the E1 sequence in p188mSZ, USF1 and Rta were no longer able to transactivate Rp, indicating that Rta autoregulates BRLF1 transcription via its interaction with USF1 on E1. This study showed that pUSF1 transfection after EBV lytic induction in P3HR1 cells increases Rta expression, indicating that USF1 activates Rta expression after the virus enters the lytic cycle. Together, these results reveal a novel mechanism by which USF interacts with Rta to promote viral lytic development, and provide additional insight into the viral-host interactions of EBV.

Published
2015

48. Hypoxia Represses ER-α Expression and Inhibits Estrogen-Induced Regulation of Ca 2+ -Activated K + Channel Activity and Myogenic Tone in Ovine Uterine Arteries

Author

Shumei Yang, Lubo Zhang, Xiang-Qun Hu, Daliao Xiao, Chiranjib Dasgupta, and Man Chen

Subjects
medicine.medical_specialty, Estrogen receptor, Biology, Decitabine, Article, Upstream Stimulatory Factor, Pregnancy, Internal medicine, Gene expression, Internal Medicine, medicine, Animals, Hypoxia, Large-Conductance Calcium-Activated Potassium Channel alpha Subunits, Promoter Regions, Genetic, Progesterone, Regulation of gene expression, Sheep, Estradiol, Estrogen Receptor alpha, Methylation, DNA Methylation, Hypoxia (medical), Acetylcysteine, Pregnancy Complications, Uterine Artery, Endocrinology, Gene Expression Regulation, DNA methylation, Azacitidine, Female, Vascular Resistance, medicine.symptom, Reactive Oxygen Species, Estrogen receptor alpha
Abstract

Previous in vivo study demonstrated that chronic hypoxia during gestation was associated with estrogen receptor-α (ER-α) gene repression in ovine uterine arteries. Yet, it remains undetermined whether hypoxia had a direct effect and if DNA methylation played a causal role in hypoxia-mediated ER-α gene repression. Thus, this study tested the hypothesis that prolonged hypoxia has a direct effect and increases promoter methylation resulting in ER-α gene repression and inhibition of estrogen-mediated adaptation of uterine vascular tone. Uterine arteries isolated from nonpregnant and pregnant sheep were treated ex vivo with 21.0% O 2 and 10.5% O 2 for 48 hours. Hypoxia significantly increased ER-α promoter methylation at both specificity protein-1 and upstream stimulatory factor binding sites, decreased specificity protein-1 and upstream stimulatory factor binding to the promoter, and suppressed ER-α expression in uterine arteries of pregnant animals. Of importance, the effects of hypoxia were blocked by a methylation inhibitor 5-aza-2′-deoxycytidine. In addition, hypoxia abrogated steroid hormone–mediated increase in ER-α expression and inhibited the hormone-induced increase in large-conductance Ca 2+ -activated K + channel activity and decrease in myogenic tone in uterine arteries of nonpregnant animals, which were reversed by 5-aza-2′-deoxycytidine. The results provide novel evidence of a direct effect of hypoxia on heightened promoter methylation that plays a causal role in ER-α gene repression and ablation of steroid hormone–mediated adaptation of uterine arterial large conductance Ca 2+ -activated K + channel activity and myogenic tone in pregnancy.

Published
2015

49. The upstream stimulatory factor USF1 is regulated by protein kinase CK2 phosphorylation

Author

Thomas Kietzmann, Claudia Götz, Tina Horbach, Sunia Khadouma, Anna-Maria Bohrer, Elitsa Y. Dimova, Sarah Lupp, and Mathias Montenarh

Subjects
Transcription, Genetic, Molecular Sequence Data, USF2, Mitogen-activated protein kinase kinase, Transfection, Upstream Stimulatory Factor, Substrate Specificity, Phosphorylation cascade, MAP2K7, Transactivation, Animals, Humans, Amino Acid Sequence, Phosphorylation, Kinase activity, Casein Kinase II, Protein Kinase Inhibitors, biology, Chemistry, Cyclin-dependent kinase 2, Cell Biology, Rats, Phosphothreonine, Biochemistry, biology.protein, Upstream Stimulatory Factors, Protein Multimerization, Holoenzymes, Plasmids, Protein Binding
Abstract

The upstream stimulatory factors 1 (USF1) and 2 (USF2) are transcription factors which bind to E-box motifs of various promoters regulating a variety of different cellular processes. Only little is known about the regulation of USFs. Here, we identified protein kinase CK2 as an enzyme that phosphorylates USF1 but not USF2. Using deletion mutants and point mutants we were able to identify threonine 100 as the major phosphorylation site for CK2. It is well known that USF1 and USF2 form hetero-dimers. Binding studies revealed that the inhibition of CK2 kinase activity by a specific inhibitor enhanced binding of USF1 to USF2. Furthermore, transactivation studies showed that the inhibition of CK2 phosphorylation of USF1 stimulated transcription from the glucokinase promoter as well as the fatty acid synthetase promoter but not from the heme oxygenase-1 promoter. Thus, we have shown for the first time that CK2 phosphorylation of USF1 modulates two functionally important properties of USF1, namely hetero-dimerization and transactivation.

Published
2014

50. The Role of HOTAIR/miR-148b-3p/USF1 on Regulating the Permeability of BTB

Author

Libo Sa, Yan Li, Lini Zhao, Yunhui Liu, Ping Wang, Libo Liu, Zhen Li, Jun Ma, Heng Cai, and Yixue Xue

Subjects
tight junction related proteins, 0301 basic medicine, Gene knockdown, Tight junction, USF1, RNA, Promoter, HOTAIR, Biology, Occludin, Upstream Stimulatory Factor, lcsh:RC321-571, 03 medical and health sciences, Cellular and Molecular Neuroscience, blood tumor barrier, 030104 developmental biology, biology.protein, Cancer research, miR-148b-3p, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Molecular Biology, Original Research, Neuroscience
Abstract

Homeobox transcript antisense intergenic RNA (HOTAIR), as a long non-coding RNA (lncRNA), has been considered to play critical roles in the biological properties of various tumors. The purposes of this study were to investigate the role and possible molecular mechanisms of HOTAIR in regulating the permeability of blood tumor barrier (BTB) in vitro. Our present study elucidated that the expressions of HOTAIR and upstream stimulatory factor 1 (USF1) was up-regulated, but miR-148b-3p was down-regulated in glioma microvascular endothelial cells (GECs). Knockdown of HOTAIR could increase the permeability of BTB as well as down-regulated the expressions of tight junction related proteins ZO-1, occludin, claudin-5, but up-regulated miR-148b-3p expressions in GECs. Meanwhile, dual-luciferase reporter assays demonstrated that HOTAIR was a target RNA of miR-148b-3p. Furthermore, overexpression of miR-148b-3p increased the permeability of BTB by down-regulating the expressions of tight junction related proteins and USF1 in GECs, and vice versa. And further result revealed USF1 was a target of miR-148b-3p. Silence of USF1 increased the permeability of BTB duo to their interaction with the promoters of ZO-1, occludin, and claudin-5 in GECs. Taken together, our finding indicated that knockdown of HOTAIR increased BTB permeability via binding to miR-148b-3p, which further reducing tight junction related proteins in GECs by targeting USF1. Thus, HOTAIR will attract more attention since it can serve as a potential target of drug delivery across BTB and may provide novel strategies for glioma treatment.

Published
2017

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