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1. Wnt3a/b-Catenin signaling conditions differentiation of partially exhausted T-effector cells in human cancers

Author

Massimo Rossi, Fabio Melandro, V. Schinzari, E. Manzi, Gian Luca Grazi, Daniela Angela Covino, Giulia Pecora, Andrea Sagnotta, Francesco Palmucci, Vincenzo Barnaba, Francesco Lancellotti, Nicola Guglielmo, Eleonora Timperi, Alessio Grimaldi, Luca Sacco, Daniela Gallerano, Piero Chirletti, Schinzari, Valeria, Timperi, Eleonora, Pecora, Giulia, Palmucci, Francesco, Gallerano, Daniela, Grimaldi, Alessio, Covino, Daniela Angela, Guglielmo, Nicola, Melandro, Fabio, Manzi, Emy, Sagnotta, Andrea, Lancellotti, Francesco, Sacco, Luca, Chirletti, Piero, Grazi, Gian Luca, Rossi, Massimo, and Barnaba, Vincenzo

Subjects
CD4-Positive T-Lymphocytes, Male, tumors, 0301 basic medicine, Cancer Research, Carcinoma, Hepatocellular, Beta-catenin, Cellular differentiation, Immunology, CD8-Positive T-Lymphocytes, Immunophenotyping, NO, cancer research, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, 0302 clinical medicine, Immune system, Wnt3A Protein, Humans, LS4_6, Wnt Signaling Pathway, beta Catenin, Aged, Aged, 80 and over, biology, Effector, Liver Neoplasms, Wnt signaling pathway, Cell Differentiation, Middle Aged, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Female, Tumor necrosis factor alpha, Colorectal Neoplasms, CD8
Abstract

In this study, we investigated the role of the Wnt/β-catenin signaling pathway in antitumor immune responses. We report that the concentration of secreted Wnt3a was significantly higher in conditioned medium from tumor or nontumor tissues obtained from all hepatocellular carcinoma or colorectal cancer patients tested, than in serum of healthy donors or patients. In addition, both Wnt3a and β-catenin were overexpressed by tumor-infiltrating and nontumor-infiltrating CD4+ or CD8+ T cells. The majority of these T cells expressed a dysfunctional effector memory Eomes+T-bet−phenotype that we defined as partially exhausted, because they performed effector functions (in terms of interferon-γ and tumor necrosis factor-α production, as well as CD107a mobilization) despite their PD-1 expression. Wnt3a/β-catenin signaling in T naïve cells in vitro recapitulated the T-cell setting in vivo. Indeed, the differentiation of cultured T naïve cells was arrested, producing cells that resembled the EomeshighT-betlowβ-cateninhigh T cells with moderate effector functions that infiltrated tumor and nontumor areas. Wnt3a blockade improved the capacity of T naïve cells to differentiate into effector cells in vitro. However, Wnt3a blockade did not affect the function and phenotype of differentiated, partially exhausted, tumor-infiltrating T cells ex vivo. Taken together, our data suggest that Wnt3a blockade halts the capacity of Wnt/β-catenin signaling to inhibit the differentiation of T naïve cells, but it does not restore the dysfunction of differentiated T cells, in the tumor setting. Cancer Immunol Res; 6(8); 941–52. ©2018 AACR.

Published
2018

2. Chronic hepatitis B virus and hepatitis C virus infections and cancer: synergy between viral and host factors

Author

Vincenzo Barnaba, Silvia Piconese, and V. Schinzari

Subjects
hepatitis C virus, Microbiology (medical), Carcinoma, Hepatocellular, Hepatitis C virus, Hepacivirus, tumours, Biology, medicine.disease_cause, Chronic liver disease, Virus, Hepatitis B, Chronic, Chronic inflammation, Hepatitis B virus, Hepatocellular carcinoma, Tumours, Infectious Diseases, medicine, Humans, Epigenetics, Liver Neoplasms, Cancer, General Medicine, hepatocellular carcinoma, Hepatitis C, Chronic, medicine.disease, Virology, 3. Good health, Immunology, Host-Pathogen Interactions, Steatohepatitis, hepatitis B virus
Abstract

Hepatitis B virus (HBV) or hepatitis C virus (HCV) infections represent major causes of chronic liver disease and hepatocellular carcinoma. Despite inducing shared pathological events leading to oncogenic transformation, these two viruses present profound differences in their molecular features, life cycle and interplay with host factors, which significantly differentiate the prognostic and therapeutic approach to the related diseases. In the present review, we report the main mechanisms involved in the multistep process leading from HCV/HBV infection and cancer development, discussing side-by-side the analogies and differences between the two viruses. Such events can be broadly categorized into (a) direct oncogenic effects, involving integration in the host genome (in the case of HBV) and chromosomal instability, interference with oncosuppressor pathways, induction of oxidative stress, promotion of angiogenesis, epithelial–mesenchymal transition, alterations in the epigenetic asset and interaction with non-coding RNAs; and (b) indirect activities mostly mediated by host events, including chronic inflammation sustained by peculiar cytokine networks (such as interleukin-6 and lymphotoxins), metabolic dysfunctions promoted by steatohepatitis, interplay with gut microbiota and fibrotic events (mainly in HCV infection). This scenario suggests that the integrated study of viral and host factors may lead to the successful development of novel biomarkers and targets for therapy.

Published
2015
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3. Dual Promoter Usage as Regulatory Mechanism of let-7c Expression in Leukemic and Solid Tumors

Author

Simona Nanni, Ruggero De Maria, Antonella Farsetti, Isabella Manni, Donatella Del Bufalo, V. Schinzari, Giulia Sagrestani, Silvia Careccia, Maria Giulia Rizzo, Maria Pia Gentileschi, Andrea Pelosi, Giulia Piaggio, Hendrik G. Stunnenberg, and Joost H.A. Martens

Subjects
Epigenomics, Cancer Research, Transcription, Genetic, Histones, Leukemia, Promyelocytic, Acute, Transcription (biology), Neoplasms, Transcriptional regulation, Promoter Regions, Genetic, Leukemic, Promyelocytic, Tumor, Leukemia, microRNA, biology, Gene Expression Regulation, Leukemic, Acetylation, Gene Expression Regulation, Neoplastic, Histone, Oncology, Transcription, Acute promyelocytic leukemia, Molecular Sequence Data, Tretinoin, Acute, Transfection, Cell Line, Promoter Regions, Genetic, Settore MED/04 - PATOLOGIA GENERALE, Cell Line, Tumor, medicine, Animals, Humans, Epigenetics, Molecular Biology, Gene, Neoplastic, Settore MED/06 - ONCOLOGIA MEDICA, Base Sequence, Promoter, medicine.disease, Introns, MicroRNAs, Gene Expression Regulation, biology.protein, Cancer research, let7-c
Abstract

Let-7c, an intronic microRNA (miRNA) embedded in the long non-coding gene LINC00478, can act as a tumor suppressor by targeting oncogenes. Previous studies indicated that in acute promyelocytic leukemia (APL), a subtype of acute myelogenous leukemia (AML) bearing the leukemia promoting PML/RARα fusion protein, let-7c expression seems to be controlled by the host gene promoter, in which canonical Retinoic Acid Responsive Elements (RAREs) are bound by PML/RARα in an all transretinoic acid (ATRA)–sensitive manner. Here, let-7c transcriptional regulation was further investigated and a novel intronic promoter upstream of the pre-miRNA was identified. This new promoter has transcriptional activity strongly indicating that at least two promoters need to be considered for let-7c transcription: the distal host gene and the proximal intronic promoter. Therefore, epigenetic modifying enzymes and histone acetylation and methylation status were analyzed on both let-7c promoters. It was demonstrated that ATRA treatment leads to let-7c upregulation inducing a more open chromatin conformation of the host gene promoter, with an enrichment of epigenetic marks that correlate with a more active transcriptional state. Conversely, the epigenetic marks on the intronic promoter are not significantly affected by ATRA treatment. Interestingly, in solid tumors such as prostate and lung adenocarcinoma it was found that both host and intronic promoters are functional. These data suggest that while the host gene promoter may control let-7c expression in AML, in a nonleukemic tumor context instead the intronic promoter contributes or preferentially regulates let-7c transcription. Implications: Alternative promoter usage represents a regulatory mechanism of let-7c expression in different tissues. Mol Cancer Res; 12(6); 878–89. ©2014 AACR.

Published
2014
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4. p53-paralog DNp73 oncogene is repressed by IFNα/STAT2 through the recruitment of the Ezh2 polycomb group transcriptional repressor

Author

Giovanni Blandino, Sabine Gerbal-Chaloin, Francesca Guerrieri, Barbara Testoni, Massimo Levrero, and V. Schinzari

Subjects
Cancer Research, Chromatin Immunoprecipitation, Blotting, Western, Methylation, Chromatin remodeling, Histones, Cell Line, Tumor, Genetics, Humans, Enhancer of Zeste Homolog 2 Protein, STAT1, Epigenetics, Promoter Regions, Genetic, Molecular Biology, Cells, Cultured, Binding Sites, biology, epigenetics, Reverse Transcriptase Polymerase Chain Reaction, Tumor Suppressor Proteins, EZH2, apoptosis, Polycomb Repressive Complex 2, Interferon-alpha, Nuclear Proteins, Promoter, STAT2 Transcription Factor, Tumor Protein p73, Hep G2 Cells, Middle Aged, Interferon-Stimulated Gene Factor 3, gamma Subunit, DNA-Binding Proteins, Histone, STAT1 Transcription Factor, Interferon-Stimulated Gene Factor 3, Colonic Neoplasms, Mutation, biology.protein, Cancer research, Hepatocytes, Original Article, chromatin dynamics, Female, RNA Interference, transcription, p53 family, Chromatin immunoprecipitation, Protein Binding, Transcription Factors
Abstract

The DNp73 proteins act as trans-repressors of p53 and p73-dependent transcription and exert both anti-apoptotic activity and pro-proliferative activity. DNp73s are frequently up-regulated in a variety of human cancers, including human hepatocellular carcinomas (HCCs). Increased levels of DNp73 proteins confer to HCC cells resistance to apoptosis and, irrespective to p53 status, a chemoresistant phenotype. Here, we show that interferon (IFN)α down-regulates DNp73 expression in primary human hepatocytes (PHHs) and HCC cell lines. IFNα has been used as pro-apoptotic agent in the treatment of malignancies and there is increasing evidence of IFNα effectiveness in HCC treatment and prevention of recurrence. The precise mechanisms by which class I IFNs exert their anti-proliferative and anti-tumor activity remain unclear. IFNα binding to its receptor activates multiple intracellular signaling cascades regulating the transcription of numerous direct target genes through the recruitment of a complex comprising of STAT1, STAT2 and IFN regulatory factor (IRF)9 to their promoters. We found that, in response to IFNα, the P2p73 promoter undergoes substantial chromatin remodeling. Histone deacetylases (HDACs) replace histone acetyl transferases. STAT2 is recruited onto the endogenous P2p73 promoter together with the polycomb group protein Ezh2, leading to increased H3K27 methylation and transcriptional repression. The reduction of DNp73 levels by IFNα is paralleled by an increased susceptibility to IFNα-triggered apoptosis of Huh7 hepatoma cells. Our results show, for the first time, that IFN-stimulated gene factor 3 recruitment may serve both in activating and repressing gene expression and identify the down-regulation of DNp73 as an additional mechanism to counteract the chemoresistance of liver cancer cells.

Published
2011

5. Human OX40 tunes the function of regulatory T cells in tumor and nontumor areas of hepatitis C virus-infected liver tissue

Author

Gianluca Mennini, Silvia Piconese, Massimo Sanchez, G. Grazi, Guido Antonelli, Vincenzo Barnaba, Massimo Rossi, Ilenia Pacella, Claudio Tripodo, Eleonora Timperi, Stefania Brozzetti, Simona Di Filippo, Katia Fazzi, Maria A ntonietta Lozzi, V. Schinzari, Nicola Guglielmo, Department of Internal Medicine and Medical Specialities, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Università degli studi di Palermo - University of Palermo, Dip di Chirurgia Generale e Trapianti d’Organo - Sapienza Università, Dipartimento di Chirurgia - Sapienza Università, Department of Molecular Medicine, Institut Pasteur, Fondation Cenci Bolognetti - Istituto Pasteur Italia, Fondazione Cenci Bolognetti, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], CISDEM-CSIC, Institute of Construction Science 'Eduardo Torreja', Réseau International des Instituts Pasteur (RIIP), This work was supported by the following grants obtained by V.B.: Associazione Italiana per la Ricerca sul Cancro (AIRC, progetto 'Investigator Grant' [IG]-2010/13 no. 10756), European Union grants (IMECS no. 201169, FP7-Health-2007-A, and SPHYNX no. 261365, FP7-Health-2010), Ministero della Sanità (Ricerca finalizzata [RFPS-2006-3-337923 and RFPS-2007-1-636647] and Istituto Superiore di Sanità [Progetto AIDS-2008]), Ministero dell’Istruzione,dell’Università e della Ricerca (MIUR, Programmi di ricerca di interesse nazionale [PRIN]-2008/10 no. 7245/1, [PRIN]-2011/13 no. 2010LC747T-004, AteneoSapienza [2009-C26A09PELN, 2010-C26A1029ZS, 2011-C26A11BYWP, and 2012-C26A12JL55], and Fondo per gli investimenti di ricerca di base [FIRB]-2011/13 no. RBAP10TPXK), Fondazione Cariplo (progetti no. 13535 and 3603 2010/12), FISM (Fondazione Italiana Sclerosi Multipla onlus) grant no. 2011/R/4, Fondazione Italiana per la Ricerca sull’Artrite (FIRA 2010), and Istituto Italiano di Tecnologia (IIT, A2 project 2013). This work was also supported bygrants obtained by S.P. from Associazione Italiana Ricerca sul Cancro (MFAG 8726) and from Ministero dell’Istruzione, dell’Università e della Ricerca (FIRB-Futuro in ricerca RBFR12I3UB_002)., The authors thank Marco Cassatella and Federica Calzetti (Università di Verona) for providing anti‐M‐DC8 antibody, Maria Cristina Gagliardi (Istituto Superiore di Sanità, Rome) for providing anti‐CD206 antibody, Carla Guarnotta (Università di Palermo) for technical assistance in immunohistochemical stainings, and Stefania Morrone ('Sapienza' Università di Roma, Rome) for help with cell sorting. The authors also acknowledge Massimo Locati and Alberto Mantovani for their helpful discussion., Piconese, Silvia, Timperi, Eleonora, Pacella, Ilenia, Schinzari, Valeria, Tripodo, Claudio, Rossi, Massimo, Guglielmo, Nicola, Mennini, Gianluca, Grazi, Gian Luca, Di Filippo, Simona, Brozzetti, Stefania, Fazzi, Katia, Antonelli, Guido, Lozzi, Maria Antonietta, Sanchez, Massimo, Barnaba, Vincenzo, Piconese, S, Timperi, E, Pacella, I, Schinzari, V, Tripodo, C, Rossi, M, Guglielmo, N, Mennini, G, Grazi, GL, Di Filippo, S, Brozzetti, S, Fazzi, K, Antonelli, G, Lozzi, MA, Sanchez, M, and Barnaba, V.

Subjects
MESH: Receptors, OX40/metabolism, MESH: Interleukin-12/metabolism, Liver Cirrhosis, Male, Macrophage, medicine.disease_cause, MESH: Carcinoma, Hepatocellular/immunology, T-Lymphocytes, Regulatory, MESH: OX40 Ligand/metabolism, 0302 clinical medicine, MESH: Aged, 80 and over, MESH: T-Lymphocytes, Regulatory/physiology, MESH: Up-Regulation, OX40, MESH: Aged, Aged, 80 and over, 0303 health sciences, education.field_of_study, T REG, MESH: Middle Aged, Medicine (all), MESH: Liver Cirrhosis/immunology, Liver Neoplasms, hemic and immune systems, Middle Aged, MESH: Liver Neoplasms/immunology, Phenotype, Hepatitis C, Interleukin-12, 3. Good health, Up-Regulation, Liver Neoplasm, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Interleukin 12, [SDV.IMM]Life Sciences [q-bio]/Immunology, Female, medicine.symptom, MESH: Hepatitis C/immunology, HEPATITIS C VIRUS, Human, medicine.medical_specialty, Carcinoma, Hepatocellular, Hepatitis C virus, Liver Cirrhosi, Population, Inflammation, chemical and pharmacologic phenomena, [SDV.CAN]Life Sciences [q-bio]/Cancer, OX40 Ligand, Biology, MESH: Phenotype, MESH: Liver Neoplasms/virology, 03 medical and health sciences, Ikaros Transcription Factor, Downregulation and upregulation, Internal medicine, medicine, Humans, MESH: Macrophages/metabolism, education, 030304 developmental biology, Aged, MESH: Humans, Hepatology, Macrophages, MESH: Carcinoma, Hepatocellular/virology, Receptors, OX40, MESH: Ikaros Transcription Factor/metabolism, MESH: Hepatitis C/complications, MESH: Male, OX40 ligand, Immunology, MESH: Liver Cirrhosis/virology, MESH: Female, 030215 immunology
Abstract

International audience; Regulatory T cells (Tregs) can be considered as a mixed population of distinct subsets, endowed with a diverse extent and quality of adaptation to microenvironmental signals. Here, we uncovered an opposite distribution of Treg expansion, phenotype, and plasticity in different microenvironments in the same organ (liver) derived from patients with chronic hepatitis C: On the one side, cirrhotic and tumor fragments were moderately and highly infiltrated by Tregs, respectively, expressing OX40 and a T-bet high IFN-c – " T-helper (Th)1-suppressing " phenotype; on the other side, noncirrhotic liver specimens contained low frequencies of Tregs that expressed low levels of OX40 and highly produced interferon-gamma (IFN-c; T-bet 1 IFN-c 1), thus becoming " Th1-like " cells. OX40-expressing and Th1-suppressing Tregs were enriched in the Helios-positive subset, carrying highly demethylated Treg cell-specific demethylated region that configures committed Tregs stably expressing forkhead box protein 3. OX40 ligand, mostly expressed by M2-like monocytes and macrophages, boosted OX40 1 Treg proliferation and antagonized the differentiation of Th1-like Tregs. However, this signal is counteracted in non-cirrhotic liver tissue (showing various levels of inflammation) by high availability of interleukin-12 and IFN-c, ultimately leading to complete, full Th1-like Treg differentiation. Conclusion: Our data demonstrate that Tregs can finely adapt, or even subvert, their classical inhibitory machinery in distinct microenvironments within the same organ. (HEPATOLOGY 2014;60:1494-1507)

Published
2014
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6. Transcriptional regulation of miR-224 upregulated in human HCCs by NFκB inflammatory pathways

Author

Melchiorre Cervello, Giuseppe Montalto, Paolo D'Onorio De Meo, Rossana De Iaco, Francesca Guerrieri, V. Schinzari, Natalia Pediconi, Giovanni Raimondo, C. Scisciani, Massimo Levrero, Teresa Pollicino, Stefania Vossio, Scisciani, C., Vossio, S., Guerrieri, F., Schinzari, V., De Iaco, R., D'Onorio De Meo, P., Cervello, M., Montalto, G., Pollicino, T., Raimondo, G., Levrero, M., and Pediconi, N.

Subjects
Lipopolysaccharides, Liver Cirrhosis, Male, Carcinoma, Hepatocellular, Transcription, Genetic, Liver Cirrhosi, Lipopolysaccharide, Biology, Cell Movement, Cell Line, Tumor, microRNA, Transcriptional regulation, Humans, NF kappa B, HCC, mir-224, nfκb, hcc, mirnas, transcription, Transcription factor, Lymphotoxin-alpha, miRNA, Aged, Hepatology, miRNAs, miR-224, Transcription, Tumor Necrosis Factor-alpha, Liver Neoplasms, NF-kappa B, MicroRNA, HCCS, Middle Aged, NFKB1, Up-Regulation, MicroRNAs, IκBα, Liver, Liver Neoplasm, Case-Control Studies, Immunology, Cancer research, Tumor necrosis factor alpha, Female, Signal transduction, Case-Control Studie, NFκB, Human, Signal Transduction
Abstract

Background & Aims: miR-224 is up-regulated in human HCCs as compared to both paired peri-tumoral cirrhotic tissues and cirrhotic livers without HCC. Here, we have cloned the miR-224 regulatory region and characterized its transcriptional regulation by the NFκB-dependent inflammatory pathways. Methods: Mature miRNA expression was evaluated by a 2 step stem-loop real-time RT-PCR. The recruitment of polymerase II and transcription factors on the pre-miR-224 promoter has been assessed by ChIPSeq and ChIP. Results: We found miR-224 levels strongly up-regulated in both peri-tumoral cirrhotic livers and HCC samples as compared to normal livers. In silico analysis of the putative miR-224 promoter revealed multiple NFκB sites. We showed that LTα and TNFα activate transcription from the miR-224 promoter and of endogenous miR-224 expression in HCC cell lines, whereas the expression of miR-224 target API5 was reduced. Exogenously expressed p65/RelA activates the miR-224 promoter and a dominant negative form of IκBα (IκBSR) represses it. ChIP analysis showed that p65/NFκB is recruited on the miR-224 promoter and that its binding sharply increases after exposure to LPS, TNFα, and LTα. Altogether these findings link the inflammatory signals to NFκB-mediated activation of miR-224 expression. An antago-miR specific for miR-224 blocked LPS and LTα stimulated HCC cells migration and invasion. Conversely, the IKK inhibitor BMS-345541 blocks pre-miR-224-induced cellular migration and invasion. Conclusions: Our results identify p65/NFκB as a direct transcriptional regulator of miR-224 expression and link miR-224 up-regulation with the activation of the LPS, LTα, and TNFα inflammatory pathways and cell migration/invasion in HCC. © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Published
2012

7. hSirT1-Dependent Regulation of the PCAF-E2F1-p73 Apoptotic Pathway in Response to DNA Damage▿

Author

Maurizio Fanciulli, Tiziana Bruno, Francesca Guerrieri, V. Schinzari, Natalia Pediconi, C. Scisciani, Stefania Vossio, Massimo Levrero, and Laura Belloni

Subjects
Transcription, Genetic, DNA damage, Apoptosis, P300-CBP Transcription Factors, Biology, Sirtuin 1, E2F1, Humans, Sirtuins, p300-CBP Transcription Factors, Promoter Regions, Genetic, Molecular Biology, Tumor Suppressor Proteins, Nuclear Proteins, Acetylation, Tumor Protein p73, Cell Biology, Articles, DNA-Binding Proteins, E2F1 Transcription Factor, Gene Expression Regulation, DNA Damage, Molecular biology, PCAF, biology.protein, NAD+ kinase, Histone deacetylase, Deacetylase activity
Abstract

The NAD(+)-dependent histone deacetylase hSirT1 regulates cell survival and stress responses by inhibiting p53-, NF-kappaB-, and E2F1-dependent transcription. Here we show that the hSirT1/PCAF interaction controls the E2F1/p73 apoptotic pathway. hSirT1 represses E2F1-dependent P1p73 promoter activity in untreated cells and inhibits its activation in response to DNA damage. hSirT1, PCAF, and E2F1 are corecruited in vivo on theP1p73 promoter. hSirT1 deacetylates PCAF in vitro and modulates PCAF acetylation in vivo. In cells exposed to apoptotic DNA damage, nuclear NAD(+) levels decrease and inactivate hSirT1 without altering the hSirT1 interaction with PCAF and hSirT1 binding to the P1p73 promoter. The reactivation of hSirT1 by pyruvate that increases the [NAD(+)]/[NADH] ratio completely abolished the DNA damage-induced activation of TAp73 expression, thus linking the modulation of chromatin-bound hSirT1 deacetylase activity by the intracellular redox state with P1p73 promoter activity. The release of PCAF from hSirT1 repression favors the assembly of transcriptionally active PCAF/E2F1 complexes onto the P1p73 promoter and p53-independent apoptosis. Our results identify hSirT1 and PCAF as potential targets to modulate tumor cell survival and chemoresistance irrespective of p53 status.

Published
2009

10. The sodium/iodide symporter NIS is a transcriptional target of the p53-family members in liver cancer cells

Author

Sabine Gerbal-Chaloin, Didier Samuel, Massimo Levrero, Silvia Piconese, Yannick Valogne, Claire Lacoste, Francesca Guerrieri, Christian Bréchot, V. Schinzari, Jamila Faivre, and Barbara Testoni

Subjects
Adult, p53, Sodium-iodide symporter, Cancer Research, Transcription, Genetic, p73, Immunology, Apoptosis, Biology, Cellular and Molecular Neuroscience, Transcription (biology), Cell Line, Tumor, Humans, Gene silencing, Gene Silencing, Promoter Regions, Genetic, Transcription factor, health care economics and organizations, Regulation of gene expression, p63, Symporters, Tumor Suppressor Proteins, Liver Neoplasms, Nuclear Proteins, Tumor Protein p73, Promoter, Cell Biology, Middle Aged, NIS, Molecular biology, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Doxorubicin, Symporter, dna damage, nis, Cancer research, DNA damage, Female, Original Article, Tumor Suppressor Protein p53, Chromatin immunoprecipitation, Protein Binding
Abstract

Thyroid iodide accumulation via the sodium/iodide symporter (NIS; SLC5A5) has been the basis for the longtime use of radio-iodide in the diagnosis and treatment of thyroid cancers. NIS is also expressed, but poorly functional, in some non-thyroid human cancers. In particular, it is much more strongly expressed in cholangiocarcinoma (CCA) and hepatocellular carcinoma (HCC) cell lines than in primary human hepatocytes (PHH). The transcription factors and signaling pathways that control NIS overexpression in these cancers is largely unknown. We identified two putative regulatory clusters of p53-responsive elements (p53REs) in the NIS core promoter, and investigated the regulation of NIS transcription by p53-family members in liver cancer cells. NIS promoter activity and endogenous NIS mRNA expression are stimulated by exogenously expressed p53-family members and significantly reduced by member-specific siRNAs. Chromatin immunoprecipitation analysis shows that the p53–REs clusters in the NIS promoter are differentially occupied by the p53-family members to regulate basal and DNA damage-induced NIS transcription. Doxorubicin strongly induces p53 and p73 binding to the NIS promoter, leading to an increased expression of endogenous NIS mRNA and protein in HCC and CCA cells, but not in PHH. Silencing NIS expression reduced doxorubicin-induced apoptosis in HCC cells, pointing to a possible role of a p53-family-dependent expression of NIS in apoptotic cell death. Altogether, these results indicate that the NIS gene is a direct target of the p53 family and suggests that the modulation of NIS by DNA-damaging agents is potentially exploitable to boost NIS upregulation in vivo.

Published
2013
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11. 310 CHROMATIN DYNAMICS OF GENES REPRESSION IN RESPONSE TO IFNa REVEAL NEW ROLES FOR STAT2, PHOSPHO-STAT2, HISTONE DEACETYLASES (HDACS) AND HISTONE METHYLATION MARKS

Author

S. Gerbal, Giovanni Blandino, Francesca Guerrieri, Massimo Levrero, Barbara Testoni, C. Voellenke, and V. Schinzari

Subjects
Hepatology, Histone H1, Histone methyltransferase, Histone H2A, EZH2, Histone methylation, Histone code, Biology, Chromatin remodeling, Cell biology, Epigenomics
Published
2011
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16. 545 THE P53-PARALOG DNP73 ONCOGENE IS REPRESSED BY α-IFN/STAT2 THROUGH THE RECRUITMENT OF YY1 AND HDAC1 TRANSCRIPTIONAL REPRESSORS

Author

V. Schinzari, Natalia Pediconi, C. Scisciani, Barbara Testoni, and Massimo Levrero

Subjects
Hepatology, biology, Chemistry, YY1, Repressor, RNA polymerase II, Molecular biology, Chromatin, Downregulation and upregulation, Transcription (biology), Interferon, biology.protein, medicine, STAT2, medicine.drug
Abstract

ackground. Expression of the p53-paralog DNp73 oncoene increases progressively in chronic hepatitis, cirrhosis nd HCC and greatly contributes to the chemoresistant henotype of HCC cells. DNp73 isoforms do not activate ranscription and do not induce apoptosis but act as domiant negative inhibitors of both p53 and TAp73. DNp73s are xpressed from the intragenic P2p73 promoter and we have ecently shown that its activity is positively regulated in heptocytes by beta-catenin and p65/NFkB. In silico analisys of he P2p73 promoter indicates that it contains two conserved SRE elements. im. To characterize the effects of -interferon on DNp73 xpression and to evaluate the functional consequences on ell proliferation and viability. ethods. Chromatin was immunoprecipatated from ntreated and IFN treated Huh7 cells with anti-AcH3, nti-STAT2, anti-P-STAT2, anti-HDAC1, anti-p300, antiY1 and anti-Pol II antibodies. DNp73 mRNA levels were uantitated real-time PCR. esults. ChIP analysis showed that both ISRE sites are ound in vivo by Stat2 and by its phosphorilated form after h of IFN treatment. Endogenous DNp73 mRNA levels re downregulated by IFN . Immunoblot analysis showed a trong DNp73 protein downregulation after IFN-treatment. hIP analysis showed that, before the IFN treatment, H3 ysines are acetylated and p300 and Pol II are bound to the 2p73 promoter, mirroring active transcription, whereas after h treatment (when the ISGF3 complex is recruited), Pol II nd p300 binding is lost whereas HDAC1, a well-known trancription cofactor related to transcriptional repression, and he YY1 co-repressor are actively recruited. These results ndicate that the recruitment of the ISGF3 complex to the 2p73promoter has a repressive activity and suggest that this h o a a isease 41 (2009) A1–A19

Published
2009
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19. Wnt3a/β-Catenin Signaling Conditions Differentiation of Partially Exhausted T-effector Cells in Human Cancers.

Author

Schinzari V, Timperi E, Pecora G, Palmucci F, Gallerano D, Grimaldi A, Covino DA, Guglielmo N, Melandro F, Manzi E, Sagnotta A, Lancellotti F, Sacco L, Chirletti P, Grazi GL, Rossi M, and Barnaba V

Subjects
Aged, Aged, 80 and over, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Cell Differentiation immunology, Female, Humans, Immunophenotyping, Male, Middle Aged, Wnt3A Protein immunology, beta Catenin metabolism, Carcinoma, Hepatocellular immunology, Colorectal Neoplasms immunology, Liver Neoplasms immunology, Lymphocytes, Tumor-Infiltrating immunology, Wnt Signaling Pathway immunology
Abstract

In this study, we investigated the role of the Wnt/β-catenin signaling pathway in antitumor immune responses. We report that the concentration of secreted Wnt3a was significantly higher in conditioned medium from tumor or nontumor tissues obtained from all hepatocellular carcinoma or colorectal cancer patients tested, than in serum of healthy donors or patients. In addition, both Wnt3a and β-catenin were overexpressed by tumor-infiltrating and nontumor-infiltrating CD4 + or CD8 + T cells. The majority of these T cells expressed a dysfunctional effector memory Eomes + T-bet - phenotype that we defined as partially exhausted, because they performed effector functions (in terms of interferon-γ and tumor necrosis factor-α production, as well as CD107a mobilization) despite their PD-1 expression. Wnt3a/β-catenin signaling in T naïve cells in vitro recapitulated the T-cell setting in vivo Indeed, the differentiation of cultured T naïve cells was arrested, producing cells that resembled the Eomes high T-bet low β-catenin high T cells with moderate effector functions that infiltrated tumor and nontumor areas. Wnt3a blockade improved the capacity of T naïve cells to differentiate into effector cells in vitro However, Wnt3a blockade did not affect the function and phenotype of differentiated, partially exhausted, tumor-infiltrating T cells ex vivo Taken together, our data suggest that Wnt3a blockade halts the capacity of Wnt/β-catenin signaling to inhibit the differentiation of T naïve cells, but it does not restore the dysfunction of differentiated T cells, in the tumor setting. Cancer Immunol Res; 6(8); 941-52. ©2018 AACR ., (©2018 American Association for Cancer Research.)

Published
2018
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20. Regulatory T cells with multiple suppressive and potentially pro-tumor activities accumulate in human colorectal cancer.

Author

Timperi E, Pacella I, Schinzari V, Focaccetti C, Sacco L, Farelli F, Caronna R, Del Bene G, Longo F, Ciardi A, Morelli S, Vestri AR, Chirletti P, Barnaba V, and Piconese S

Abstract

Tregs can contribute to tumor progression by suppressing antitumor immunity. Exceptionally, in human colorectal cancer (CRC), Tregs are thought to exert beneficial roles in controlling pro-tumor chronic inflammation. The goal of our study was to characterize CRC-infiltrating Tregs at multiple levels, by phenotypical, molecular and functional evaluation of Tregs from the tumor site, compared to non-tumoral mucosa and peripheral blood of CRC patients. The frequency of Tregs was higher in mucosa than in blood, and further significantly increased in tumor. Ex vivo, those Tregs suppressed the proliferation of tumor-infiltrating CD8(+) and CD4(+) T cells. A differential compartmentalization was detected between Helios(high) and Helios(low) Treg subsets (thymus-derived versus peripherally induced): while Helios(low) Tregs were enriched in both sites, only Helios(high) Tregs accumulated significantly and specifically in tumors, displayed a highly demethylated TSDR region and contained high proportions of cells expressing CD39 and OX40, markers of activation and suppression. Besides the suppression of T cells, Tregs may contribute to CRC progression also through releasing IL-17, or differentiating into Tfr cells that potentially antagonize a protective Tfh response, events that were both detected in tumor-associated Tregs. Overall, our data indicate that Treg accumulation may contribute through multiple mechanisms to CRC establishment and progression.

Published
2016
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21. Chronic hepatitis B virus and hepatitis C virus infections and cancer: synergy between viral and host factors.

Author

Schinzari V, Barnaba V, and Piconese S

Subjects
Carcinoma, Hepatocellular epidemiology, Hepacivirus physiology, Hepatitis B virus physiology, Humans, Liver Neoplasms epidemiology, Carcinoma, Hepatocellular pathology, Hepacivirus pathogenicity, Hepatitis B virus pathogenicity, Hepatitis B, Chronic complications, Hepatitis C, Chronic complications, Host-Pathogen Interactions, Liver Neoplasms pathology
Abstract

Hepatitis B virus (HBV) or hepatitis C virus (HCV) infections represent major causes of chronic liver disease and hepatocellular carcinoma. Despite inducing shared pathological events leading to oncogenic transformation, these two viruses present profound differences in their molecular features, life cycle and interplay with host factors, which significantly differentiate the prognostic and therapeutic approach to the related diseases. In the present review, we report the main mechanisms involved in the multistep process leading from HCV/HBV infection and cancer development, discussing side-by-side the analogies and differences between the two viruses. Such events can be broadly categorized into (a) direct oncogenic effects, involving integration in the host genome (in the case of HBV) and chromosomal instability, interference with oncosuppressor pathways, induction of oxidative stress, promotion of angiogenesis, epithelial-mesenchymal transition, alterations in the epigenetic asset and interaction with non-coding RNAs; and (b) indirect activities mostly mediated by host events, including chronic inflammation sustained by peculiar cytokine networks (such as interleukin-6 and lymphotoxins), metabolic dysfunctions promoted by steatohepatitis, interplay with gut microbiota and fibrotic events (mainly in HCV infection). This scenario suggests that the integrated study of viral and host factors may lead to the successful development of novel biomarkers and targets for therapy., (Copyright © 2015 European Society of Clinical Microbiology and Infectious Diseases. Published by Elsevier Ltd. All rights reserved.)

Published
2015
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22. Human OX40 tunes the function of regulatory T cells in tumor and nontumor areas of hepatitis C virus-infected liver tissue.

Author

Piconese S, Timperi E, Pacella I, Schinzari V, Tripodo C, Rossi M, Guglielmo N, Mennini G, Grazi GL, Di Filippo S, Brozzetti S, Fazzi K, Antonelli G, Lozzi MA, Sanchez M, and Barnaba V

Subjects
Aged, Aged, 80 and over, Carcinoma, Hepatocellular virology, Female, Hepatitis C complications, Humans, Ikaros Transcription Factor metabolism, Interleukin-12 metabolism, Liver Cirrhosis virology, Liver Neoplasms virology, Macrophages metabolism, Male, Middle Aged, OX40 Ligand metabolism, Phenotype, Up-Regulation, Carcinoma, Hepatocellular immunology, Hepatitis C immunology, Liver Cirrhosis immunology, Liver Neoplasms immunology, Receptors, OX40 metabolism, T-Lymphocytes, Regulatory physiology
Abstract

Unlabelled: Regulatory T cells (Tregs) can be considered as a mixed population of distinct subsets, endowed with a diverse extent and quality of adaptation to microenvironmental signals. Here, we uncovered an opposite distribution of Treg expansion, phenotype, and plasticity in different microenvironments in the same organ (liver) derived from patients with chronic hepatitis C: On the one side, cirrhotic and tumor fragments were moderately and highly infiltrated by Tregs, respectively, expressing OX40 and a T-bethigh IFN-γ- "T-helper (Th)1-suppressing" phenotype; on the other side, noncirrhotic liver specimens contained low frequencies of Tregs that expressed low levels of OX40 and highly produced interferon-gamma (IFN-γ; T-bet+IFN-γ+), thus becoming "Th1-like" cells. OX40-expressing and Th1-suppressing Tregs were enriched in the Helios-positive subset, carrying highly demethylated Treg cell-specific demethylated region that configures committed Tregs stably expressing forkhead box protein 3. OX40 ligand, mostly expressed by M2-like monocytes and macrophages, boosted OX40+ Treg proliferation and antagonized the differentiation of Th1-like Tregs. However, this signal is counteracted in noncirrhotic liver tissue (showing various levels of inflammation) by high availability of interleukin-12 and IFN-γ, ultimately leading to complete, full Th1-like Treg differentiation., Conclusion: Our data demonstrate that Tregs can finely adapt, or even subvert, their classical inhibitory machinery in distinct microenvironments within the same organ., (© 2014 by the American Association for the Study of Liver Diseases.)

Published
2014
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23. Dual promoter usage as regulatory mechanism of let-7c expression in leukemic and solid tumors.

Author

Pelosi A, Careccia S, Sagrestani G, Nanni S, Manni I, Schinzari V, Martens JH, Farsetti A, Stunnenberg HG, Gentileschi MP, Del Bufalo D, De Maria R, Piaggio G, and Rizzo MG

Subjects
Acetylation, Animals, Base Sequence, Cell Line, Tumor, Epigenomics, Gene Expression Regulation, Leukemic, Gene Expression Regulation, Neoplastic, Histones genetics, Histones metabolism, Humans, Introns, Leukemia metabolism, Leukemia, Promyelocytic, Acute genetics, MicroRNAs genetics, Molecular Sequence Data, Neoplasms metabolism, Promoter Regions, Genetic, Transcription, Genetic, Transfection, Tretinoin pharmacology, Leukemia genetics, Leukemia, Promyelocytic, Acute metabolism, MicroRNAs biosynthesis, Neoplasms genetics
Abstract

Unlabelled: Let-7c, an intronic microRNA (miRNA) embedded in the long non-coding gene LINC00478, can act as a tumor suppressor by targeting oncogenes. Previous studies indicated that in acute promyelocytic leukemia (APL), a subtype of acute myelogenous leukemia (AML) bearing the leukemia promoting PML/RARα fusion protein, let-7c expression seems to be controlled by the host gene promoter, in which canonical Retinoic Acid Responsive Elements (RAREs) are bound by PML/RARα in an all transretinoic acid (ATRA)-sensitive manner. Here, let-7c transcriptional regulation was further investigated and a novel intronic promoter upstream of the pre-miRNA was identified. This new promoter has transcriptional activity strongly indicating that at least two promoters need to be considered for let-7c transcription: the distal host gene and the proximal intronic promoter. Therefore, epigenetic modifying enzymes and histone acetylation and methylation status were analyzed on both let-7c promoters. It was demonstrated that ATRA treatment leads to let-7c upregulation inducing a more open chromatin conformation of the host gene promoter, with an enrichment of epigenetic marks that correlate with a more active transcriptional state. Conversely, the epigenetic marks on the intronic promoter are not significantly affected by ATRA treatment. Interestingly, in solid tumors such as prostate and lung adenocarcinoma it was found that both host and intronic promoters are functional. These data suggest that while the host gene promoter may control let-7c expression in AML, in a nonleukemic tumor context instead the intronic promoter contributes or preferentially regulates let-7c transcription., Implications: Alternative promoter usage represents a regulatory mechanism of let-7c expression in different tissues. Mol Cancer Res; 12(6); 878-89. ©2014 AACR., (©2014 American Association for Cancer Research.)

Published
2014
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24. The sodium/iodide symporter NIS is a transcriptional target of the p53-family members in liver cancer cells.

Author

Guerrieri F, Piconese S, Lacoste C, Schinzari V, Testoni B, Valogne Y, Gerbal-Chaloin S, Samuel D, Bréchot C, Faivre J, and Levrero M

Subjects
Adult, Apoptosis drug effects, Apoptosis genetics, Cell Line, Tumor, DNA Damage genetics, Doxorubicin pharmacology, Female, Gene Expression Regulation, Neoplastic drug effects, Gene Silencing drug effects, Humans, Liver Neoplasms pathology, Middle Aged, Promoter Regions, Genetic genetics, Protein Binding drug effects, Protein Binding genetics, Symporters metabolism, Tumor Protein p73, DNA-Binding Proteins metabolism, Liver Neoplasms genetics, Nuclear Proteins metabolism, Symporters genetics, Transcription, Genetic drug effects, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Proteins metabolism
Abstract

Thyroid iodide accumulation via the sodium/iodide symporter (NIS; SLC5A5) has been the basis for the longtime use of radio-iodide in the diagnosis and treatment of thyroid cancers. NIS is also expressed, but poorly functional, in some non-thyroid human cancers. In particular, it is much more strongly expressed in cholangiocarcinoma (CCA) and hepatocellular carcinoma (HCC) cell lines than in primary human hepatocytes (PHH). The transcription factors and signaling pathways that control NIS overexpression in these cancers is largely unknown. We identified two putative regulatory clusters of p53-responsive elements (p53REs) in the NIS core promoter, and investigated the regulation of NIS transcription by p53-family members in liver cancer cells. NIS promoter activity and endogenous NIS mRNA expression are stimulated by exogenously expressed p53-family members and significantly reduced by member-specific siRNAs. Chromatin immunoprecipitation analysis shows that the p53-REs clusters in the NIS promoter are differentially occupied by the p53-family members to regulate basal and DNA damage-induced NIS transcription. Doxorubicin strongly induces p53 and p73 binding to the NIS promoter, leading to an increased expression of endogenous NIS mRNA and protein in HCC and CCA cells, but not in PHH. Silencing NIS expression reduced doxorubicin-induced apoptosis in HCC cells, pointing to a possible role of a p53-family-dependent expression of NIS in apoptotic cell death. Altogether, these results indicate that the NIS gene is a direct target of the p53 family and suggests that the modulation of NIS by DNA-damaging agents is potentially exploitable to boost NIS upregulation in vivo.

Published
2013
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25. Induction, control, and plasticity of Treg cells: the immune regulatory network revised?

Author

Barnaba V and Schinzari V

Subjects
Animals, Autoimmunity immunology, Forkhead Transcription Factors immunology, Homeostasis immunology, Humans, Immune Tolerance immunology, Infections immunology, Inflammation immunology, Neoplasms immunology, T-Lymphocytes, Regulatory cytology, T-Lymphocytes, Regulatory immunology
Abstract

Treg cells expressing the Foxp3 transcription factor play a key role in several aspects of immunological tolerance and in the establishment of immune homeostasis. Here, we discuss the mechanisms, including new evidence on the signals required by Tconv cells to convert into Treg cells described by Yao and colleagues [Eur. J. Immunol. 2013. 43: 458-467] in this issue of European Journal of Immunology, by which Treg-cell dynamics, plasticity and diversification correlate with diverse functions (induction, suppression, contra-suppression) in a variety of settings, such as inflammation, chronic infections, cancer, and autoimmunity., (© 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published
2013
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26. Transcriptional regulation of miR-224 upregulated in human HCCs by NFκB inflammatory pathways.

Author

Scisciani C, Vossio S, Guerrieri F, Schinzari V, De Iaco R, D'Onorio de Meo P, Cervello M, Montalto G, Pollicino T, Raimondo G, Levrero M, and Pediconi N

Subjects
Aged, Carcinoma, Hepatocellular pathology, Case-Control Studies, Cell Line, Tumor, Cell Movement drug effects, Female, Humans, Lipopolysaccharides pharmacology, Liver pathology, Liver physiology, Liver Cirrhosis pathology, Liver Cirrhosis physiopathology, Liver Neoplasms pathology, Lymphotoxin-alpha pharmacology, Male, Middle Aged, Tumor Necrosis Factor-alpha pharmacology, Carcinoma, Hepatocellular physiopathology, Liver Neoplasms physiopathology, MicroRNAs physiology, NF-kappa B physiology, Signal Transduction physiology, Transcription, Genetic physiology, Up-Regulation physiology
Abstract

Background & Aims: miR-224 is up-regulated in human HCCs as compared to both paired peri-tumoral cirrhotic tissues and cirrhotic livers without HCC. Here, we have cloned the miR-224 regulatory region and characterized its transcriptional regulation by the NFκB-dependent inflammatory pathways., Methods: Mature miRNA expression was evaluated by a 2 step stem-loop real-time RT-PCR. The recruitment of polymerase II and transcription factors on the pre-miR-224 promoter has been assessed by ChIPSeq and ChIP., Results: We found miR-224 levels strongly up-regulated in both peri-tumoral cirrhotic livers and HCC samples as compared to normal livers. In silico analysis of the putative miR-224 promoter revealed multiple NFκB sites. We showed that LTα and TNFα activate transcription from the miR-224 promoter and of endogenous miR-224 expression in HCC cell lines, whereas the expression of miR-224 target API5 was reduced. Exogenously expressed p65/RelA activates the miR-224 promoter and a dominant negative form of IκBα (IκBSR) represses it. ChIP analysis showed that p65/NFκB is recruited on the miR-224 promoter and that its binding sharply increases after exposure to LPS, TNFα, and LTα. Altogether these findings link the inflammatory signals to NFκB-mediated activation of miR-224 expression. An antago-miR specific for miR-224 blocked LPS and LTα stimulated HCC cells migration and invasion. Conversely, the IKK inhibitor BMS-345541 blocks pre-miR-224-induced cellular migration and invasion., Conclusions: Our results identify p65/NFκB as a direct transcriptional regulator of miR-224 expression and link miR-224 up-regulation with the activation of the LPS, LTα, and TNFα inflammatory pathways and cell migration/invasion in HCC., (Copyright © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published
2012
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27. p53-paralog DNp73 oncogene is repressed by IFNα/STAT2 through the recruitment of the Ezh2 polycomb group transcriptional repressor.

Author

Testoni B, Schinzari V, Guerrieri F, Gerbal-Chaloin S, Blandino G, and Levrero M

Subjects
Binding Sites genetics, Blotting, Western, Cell Line, Tumor, Cells, Cultured, Chromatin Immunoprecipitation, Colonic Neoplasms genetics, Colonic Neoplasms metabolism, Colonic Neoplasms pathology, DNA-Binding Proteins genetics, Enhancer of Zeste Homolog 2 Protein, Female, Hep G2 Cells, Hepatocytes drug effects, Hepatocytes metabolism, Histones metabolism, Humans, Interferon-Stimulated Gene Factor 3, gamma Subunit genetics, Interferon-Stimulated Gene Factor 3, gamma Subunit metabolism, Interferon-alpha metabolism, Methylation drug effects, Middle Aged, Mutation, Nuclear Proteins genetics, Polycomb Repressive Complex 2, Promoter Regions, Genetic genetics, Protein Binding drug effects, RNA Interference, Reverse Transcriptase Polymerase Chain Reaction, STAT1 Transcription Factor genetics, STAT1 Transcription Factor metabolism, STAT2 Transcription Factor genetics, Transcription Factors genetics, Tumor Protein p73, Tumor Suppressor Proteins genetics, DNA-Binding Proteins metabolism, Interferon-alpha pharmacology, Nuclear Proteins metabolism, STAT2 Transcription Factor metabolism, Transcription Factors metabolism, Tumor Suppressor Proteins metabolism
Abstract

The DNp73 proteins act as trans-repressors of p53 and p73-dependent transcription and exert both anti-apoptotic activity and pro-proliferative activity. DNp73s are frequently up-regulated in a variety of human cancers, including human hepatocellular carcinomas (HCCs). Increased levels of DNp73 proteins confer to HCC cells resistance to apoptosis and, irrespective to p53 status, a chemoresistant phenotype. Here, we show that interferon (IFN)α down-regulates DNp73 expression in primary human hepatocytes (PHHs) and HCC cell lines. IFNα has been used as pro-apoptotic agent in the treatment of malignancies and there is increasing evidence of IFNα effectiveness in HCC treatment and prevention of recurrence. The precise mechanisms by which class I IFNs exert their anti-proliferative and anti-tumor activity remain unclear. IFNα binding to its receptor activates multiple intracellular signaling cascades regulating the transcription of numerous direct target genes through the recruitment of a complex comprising of STAT1, STAT2 and IFN regulatory factor (IRF)9 to their promoters. We found that, in response to IFNα, the P2p73 promoter undergoes substantial chromatin remodeling. Histone deacetylases (HDACs) replace histone acetyl transferases. STAT2 is recruited onto the endogenous P2p73 promoter together with the polycomb group protein Ezh2, leading to increased H3K27 methylation and transcriptional repression. The reduction of DNp73 levels by IFNα is paralleled by an increased susceptibility to IFNα-triggered apoptosis of Huh7 hepatoma cells. Our results show, for the first time, that IFN-stimulated gene factor 3 recruitment may serve both in activating and repressing gene expression and identify the down-regulation of DNp73 as an additional mechanism to counteract the chemoresistance of liver cancer cells.

Published
2011
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28. hSirT1-dependent regulation of the PCAF-E2F1-p73 apoptotic pathway in response to DNA damage.

Author

Pediconi N, Guerrieri F, Vossio S, Bruno T, Belloni L, Schinzari V, Scisciani C, Fanciulli M, and Levrero M

Subjects
Acetylation, Gene Expression Regulation, Humans, Promoter Regions, Genetic, Sirtuin 1, Transcription, Genetic, Tumor Protein p73, Apoptosis, DNA Damage, DNA-Binding Proteins metabolism, E2F1 Transcription Factor metabolism, Nuclear Proteins metabolism, Sirtuins physiology, Tumor Suppressor Proteins metabolism, p300-CBP Transcription Factors metabolism
Abstract

The NAD(+)-dependent histone deacetylase hSirT1 regulates cell survival and stress responses by inhibiting p53-, NF-kappaB-, and E2F1-dependent transcription. Here we show that the hSirT1/PCAF interaction controls the E2F1/p73 apoptotic pathway. hSirT1 represses E2F1-dependent P1p73 promoter activity in untreated cells and inhibits its activation in response to DNA damage. hSirT1, PCAF, and E2F1 are corecruited in vivo on theP1p73 promoter. hSirT1 deacetylates PCAF in vitro and modulates PCAF acetylation in vivo. In cells exposed to apoptotic DNA damage, nuclear NAD(+) levels decrease and inactivate hSirT1 without altering the hSirT1 interaction with PCAF and hSirT1 binding to the P1p73 promoter. The reactivation of hSirT1 by pyruvate that increases the [NAD(+)]/[NADH] ratio completely abolished the DNA damage-induced activation of TAp73 expression, thus linking the modulation of chromatin-bound hSirT1 deacetylase activity by the intracellular redox state with P1p73 promoter activity. The release of PCAF from hSirT1 repression favors the assembly of transcriptionally active PCAF/E2F1 complexes onto the P1p73 promoter and p53-independent apoptosis. Our results identify hSirT1 and PCAF as potential targets to modulate tumor cell survival and chemoresistance irrespective of p53 status.

Published
2009
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