Your search keyword '"Laura Ciudad"' showing total 19 results

1. MAFB surrogates the glucocorticoid receptor ability to induce tolerogenesis in dendritic cells

Author

Miranda Houtman, Caroline Ospelt, Carlos de la Calle-Fabregat, Gisela Barbisan, Octavio Morante-Palacios, Tianlu Li, Mojca Frank-Bertoncelj, Raphael Micheroli, Esteban Ballestar, Sam Edalat, and Laura Ciudad

Subjects

Transcriptome, Gene knockdown, DNA demethylation, Glucocorticoid receptor, Immune system, Downregulation and upregulation, MAFB, Biology, Epigenomics, Cell biology

Abstract

Glucocorticoids (GCs) exert potent anti-inflammatory effects in immune cells through the glucocorticoid receptor (GR). Dendritic cells (DCs), central actors for coordinating immune responses, acquire tolerogenic properties in response to GCs. Tolerogenic DCs (tolDCs) have emerged as a potential treatment for various inflammatory diseases. To date, the underlying cell type-specific regulatory mechanisms orchestrating GC-mediated acquisition of immunosuppressive properties remain poorly understood. In this study, we investigated the transcriptomic and epigenomic remodeling associated with differentiation to DCs in the presence of GCs. Our analysis demonstrates a major role of MAFB in this process, in synergy with GR. GR and MAFB both interact with methylcytosine dioxygenase TET2 and bind to genomic loci that undergo specific demethylation in tolDCs. We also show that the role of MAFB is more extensive, binding to thousands of genomic loci in tolDCs. Finally, MAFB knockdown erases the tolerogenic properties of tolDCs and reverts the specific DNA demethylation and gene upregulation. The preeminent role of MAFB is also demonstrated in vivo for myeloid cells from synovium in rheumatoid arthritis following GC treatment. Our results imply that, once directly activated by GR, MAFB takes over the main roles to orchestrate the epigenomic and transcriptomic remodeling that define the tolerogenic phenotype.

Published

2021

2. Activation-induced deaminase is critical for the establishment of DNA methylation patterns prior to the germinal center reaction

Author

Dieter Weichenhan, Tianlu Li, Felipe Prosper, Sven Kracker, Pere Soler-Palacín, Lennart Hammarström, Andrea Martín-Nalda, Javier Rodríguez-Ubreva, Anne Durandy, Mónica Martínez-Gallo, Romina Dieli-Crimi, Anna G. Ferreté-Bonastre, Pavlo Lutsik, Ángel F. Álvarez-Prado, Laura Ciudad, Bodo Grimbacher, Jacques G. Rivière, Carsten Speckmann, Christoph Plass, Esteban Ballestar, Christian Klemann, Amaya Vilas-Zornoza, Hassan Abolhassani, Francesc Català-Moll, Roger Colobran, Institut Català de la Salut, [Català-Moll F, Ferreté-Bonastre AG, Li T, Ciudad L] Epigenetics and Immune Disease Group, Josep Carreras Research Institute (IJC), 08916 Badalona, Barcelona, Spain. Chromatin and Disease Group, Cancer Epigenetics and Biology Programme (PEBC), Bellvitge Biomedical Research Institute (IDIBELL), 08908 L’Hospitalet de Llobregat, Barcelona, Spain. [Weichenhan D, Lutsik P] Division of Cancer Epigenomics, German Cancer Research Center (DKFZ), Heidelberg 69120, Germany. [Martínez-Gallo M, Dieli-Crimi R] Divisió d’Immunologia, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Grup de Recerca en Immunologia Diagnòstica, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. [Rivière JG, Martín-Nalda A, Soler-Palacín P] Unitat de Patologia Infecciosa i Immunodeficiències de Pediatria, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Grup de Recerca d’Infecció en els Pacients Pediàtrics Immunodeprimits, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Vall d’Hebron Hospital Universitari, Barcelona, Spain. Jeffrey Modell Diagnostic and Research Center for Primary Immunodeficiencies, Barcelona, Spain. [Colobran R] Divisió d’Immunologia, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Grup de Recerca en Immunologia Diagnòstica, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Jeffrey Modell Diagnostic and Research Center for Primary Immunodeficiencies, Barcelona, Spain. Departament de Biologia Cel·lular, Fisiologia i Immunologia, Universitat Autònoma de Barcelona, Bellaterra, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

AcademicSubjects/SCI00010, Bisulfite sequencing, ADN, Autoimmunity, Cèl·lules B - Immunologia, Hyper-IgM Immunodeficiency Syndrome, 0302 clinical medicine, AID, Activation-induced (cytidine) deaminase, Otros calificadores::Otros calificadores::/inmunología [Otros calificadores], 0303 health sciences, B-Lymphocytes, ADN - Metilació, medicine.anatomical_structure, células::células::células sanguíneas::leucocitos::leucocitos mononucleares::linfocitos::linfocitos B [ANATOMÍA], DNA methylation, Metilació, Rearrangements, Sequencing reveals, Cèl·lules B, Investigative Techniques::Genetic Techniques::Sequence Analysis::Sequence Analysis, DNA::Whole Genome Sequencing [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Naive B cell, Somatic hypermutation, Receptors, Antigen, B-Cell, Biology, Methylation, Cells::Antibody-Producing Cells::B-Lymphocytes [ANATOMY], 03 medical and health sciences, técnicas de investigación::técnicas genéticas::análisis de secuencias::análisis de secuencias de ADN::secuenciación del genoma completo [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Other subheadings::Other subheadings::/immunology [Other subheadings], B-Cell receptor, Cytidine Deaminase, Genetics, medicine, Immune Tolerance, Humans, B cell, Seqüència de nucleòtids, 030304 developmental biology, B cells, Genetic Phenomena::DNA Methylation [PHENOMENA AND PROCESSES], Whole Genome Sequencing, Hypermutation, Gene regulation, Chromatin and Epigenetics, Germinal center, fenómenos genéticos::metilación del ADN [FENÓMENOS Y PROCESOS], DNA, DNA Methylation, Germinal Center, Molecular biology, Induced cytidine deaminase, Demethylation, Super-enhancers, DNA demethylation, biology.protein, Transcription factor, Class-switch recombination, Transcriptome, Immunologic Memory, 030217 neurology & neurosurgery

Abstract

Limfòcits b; Metilació de l'ADN; Genoma Linfocitos b; Metilación de ADN; Genoma B-lymphocytes; DNA methylation; Genome Activation-induced deaminase (AID) initiates antibody diversification in germinal center B cells by deaminating cytosines, leading to somatic hypermutation and class-switch recombination. Loss-of-function mutations in AID lead to hyper-IgM syndrome type 2 (HIGM2), a rare human primary antibody deficiency. AID-mediated deamination has been proposed as leading to active demethylation of 5-methycytosines in the DNA, although evidence both supports and casts doubt on such a role. In this study, using whole-genome bisulfite sequencing of HIGM2 B cells, we investigated direct AID involvement in active DNA demethylation. HIGM2 naïve and memory B cells both display widespread DNA methylation alterations, of which ∼25% are attributable to active DNA demethylation. For genes that undergo active demethylation that is impaired in HIGM2 individuals, our analysis indicates that AID is not directly involved. We demonstrate that the widespread alterations in the DNA methylation and expression profiles of HIGM2 naïve B cells result from premature overstimulation of the B-cell receptor prior to the germinal center reaction. Our data support a role for AID in B cell central tolerance in preventing the expansion of autoreactive cell clones, affecting the correct establishment of DNA methylation patterns. Spanish Ministry of Science, Innovation and Universities [SAF2017-88086-R to E.B.]; cofunded by FEDER funds/European Regional Development Fund (ERDF)—a way to build Europe. E.B is supported by Instituto de Salud Carlos III (ISCIII), Ref. AC18/00057, associated with i-PAD project (ERARE European Union program); P.L. and C.P. are supported by the German Cancer Aid project CO-CLL [70113869]; B.G. is funded by the Deutsche Forschungsgemeinschaft [GR1617/14-1/iPAD, SFB1160/2_B5, RESIST–EXC 2155–Project ID 390874280, CIBSS–EXC-2189–Project ID 390939984]; BMBF [GAIN 01GM1910A]. Funding for open access charge: Spanish Ministry of Science, Innovation and Universities [SAF2017-88086-R].

Published

2021

3. Targeting aberrant DNA methylation in mesenchymal stromal cells as a treatment for myeloma bone disease

Author

Antonio Garcia-Gomez, Laura San-Segundo, Laura Ciudad, Manel Esteller, Xabier Morales, Esteban Ballestar, Javier Rodríguez-Ubreva, Carlos Ortiz-de-Solorzano, Julen Oyarzabal, Felipe Prosper, Mercedes Garayoa, Tianlu Li, Sandra Muntión, Montserrat Martín-Sánchez, Xabier Agirre, Edurne San José-Enériz, Carlos de la Calle-Fabregat, Gerard Godoy-Tena, Francesc Català-Moll, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Multiple Myeloma Research Foundation, European Commission, Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, Fundació La Marató de TV3, Associazione Italiana per la Ricerca sul Cancro, and Fundación Ramón Areces

Subjects

0301 basic medicine, Male, Bone disease, ADN, General Physics and Astronomy, Myeloma, Epigenesis, Genetic, Mice, 0302 clinical medicine, Bone Marrow, Osteogenesis, Multiple myeloma, Histocompatibility Antigens, DNA (Cytosine-5-)-Methyltransferases, Femur, Enzyme Inhibitors, Regulation of gene expression, Aged, 80 and over, Multidisciplinary, DNA methylation, Osteoblast, Middle Aged, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Female, Bone Diseases, Multiple Myeloma, Adult, Science, Antineoplastic Agents, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Target identification, medicine, Animals, Humans, Epigenetics, Aged, Mesenchymal stem cell, Mieloma múltiple, Mesenchymal Stem Cells, General Chemistry, Histone-Lysine N-Methyltransferase, DNA, DNA Methylation, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, Cancer research, Bone marrow

Abstract

© The Author(s) 2021., Multiple myeloma (MM) progression and myeloma-associated bone disease (MBD) are highly dependent on bone marrow mesenchymal stromal cells (MSCs). MM-MSCs exhibit abnormal transcriptomes, suggesting the involvement of epigenetic mechanisms governing their tumor-promoting functions and prolonged osteoblast suppression. Here, we identify widespread DNA methylation alterations of bone marrow-isolated MSCs from distinct MM stages, particularly in Homeobox genes involved in osteogenic differentiation that associate with their aberrant expression. Moreover, these DNA methylation changes are recapitulated in vitro by exposing MSCs from healthy individuals to MM cells. Pharmacological targeting of DNMTs and G9a with dual inhibitor CM-272 reverts the expression of hypermethylated osteogenic regulators and promotes osteoblast differentiation of myeloma MSCs. Most importantly, CM-272 treatment prevents tumor-associated bone loss and reduces tumor burden in a murine myeloma model. Our results demonstrate that epigenetic aberrancies mediate the impairment of bone formation in MM, and its targeting by CM-272 is able to reverse MBD., We thank CERCA Program/Generalitat de Catalunya and the Josep Carreras Foundation for institutional support. E.B. was funded by the Spanish Ministry of Science and Innovation (grant numbers SAF2014-55942-R and SAF2017-88086-R), co-funded by FEDER funds/European Regional Development Fund (ERDF)—a way to build Europe, and a Senior Research Award from the Multiple Myeloma Research Foundation (MMRF). C.O.-d.-S. was funded by the Spanish Ministry of Science, Innovation and Universities, under grant RTI2018-094494-B-C22 (MCIU/AEI/FEDER, UE). M.G. received financial support from the Spanish FIS-ISCIII (PI15/02156 and PI19/01384) and FEDER. A.G.G is funded by a postdoctoral contract of the Asociación Española Contra el Cáncer (AECC). F.P. was funded by grants from Instituto de Salud Carlos III (ISCIII), PI17/00701 and PI19/01352, TRASCAN (EPICA and Immunocell), Fundació La Marató de TV3, the Accelerator award CRUK/AIRC/AECC joint funder-partnership, CIBERONC (CB16/12/00489) and co-financed with FEDER funds and Fundación Ramón Areces (PREMAMM).

Published

2021

4. Vitamin D Receptor, STAT3 and TET2 Cooperate to Establish Tolerogenesis

Author

Javier Rodríguez-Ubreva, Laura Barberà, Octavio Morante-Palacios, Anna G. Ferreté-Bonastre, Francesc Català-Moll, Federico Fondelli, Gerard Godoy-Tena, Esteban Ballestar, Eva Martínez-Cáceres, Tianlu Li, and Laura Ciudad

Subjects

STAT3 Transcription Factor, Tolerogenesis, Dendritic cells, Calcitriol receptor, General Biochemistry, Genetics and Molecular Biology, Dioxygenases, STAT3, Immune Tolerance, Vitamin D and neurology, Humans, Epigenetics, Vitamin D, Cells, Cultured, VDR, Epigenomics, TET2, DNA methylation, biology, Chemistry, Dendritic Cells, Cell biology, DNA-Binding Proteins, Methylcytosine Dioxygenase TET2, DNA demethylation, JAK2, biology.protein, Receptors, Calcitriol, Phosphorylation, IL-6-JAK-STAT

Abstract

We are very grateful to Dr. José Luis Sardina for useful feedback. We thank CERCA Programme/Generalitat de Catalunya and the Josep Carreras Foundation for institutional support. E.B. was funded by the Spanish Ministry of Science and Innovation (MICINN ; grant number PID2020-117212RB-I00/AEI/10.13038/501100011033). E.M.-C. is funded with RESTORE project (EU H2020 Research and Innovation Programme, number 779316) and Spanish projects PI17/01521 and PI20/01313, integrated in the Plan Nacional de I+D+I and co-supported by the ISCIII-Subdirección General de Evaluación and FEDER. O.M.-P. holds an i-PFIS PhD fellowship (grant number IFI17/00034) from Acción Estratégica en Salud 2013-2016 ISCIII, co-financed by Fondo Social Europeo. F.F. holds a PhD fellowship from the INsTRuCT Consortium, which receives. Innovative Training Network subsidy from the EU H2020 program. We are very grateful to Dr. Jos? Luis Sardina for useful feedback. We thank CERCA Programme/Generalitat de Catalunya and the Josep Carreras Foundation for institutional support. E.B. was funded by the Spanish Ministry of Science and Innovation (MICINN; grant number PID2020-117212RB-I00/AEI/10.13038/501100011033). E.M.-C. is funded with RESTORE project (EU H2020 Research and Innovation Programme, number 779316) and Spanish projects PI17/01521 and PI20/01313, integrated in the Plan Nacional de I+D+I and co-supported by the ISCIII-Subdirecci?n General de Evaluaci?n and FEDER. O.M.-P. holds an i-PFIS PhD fellowship (grant number IFI17/00034) from Acci?n Estrat?gica en Salud 2013?2016 ISCIII, co-financed by Fondo Social Europeo. F.F. holds a PhD fellowship from the INsTRuCT Consortium, which receives. Innovative Training Network subsidy from the EU H2020 program. F.C.-M. and E.B. conceived and designed the study; F.C.-M. A.G.F.-B. G.G.-T. O.M.-P. L.C. L.B. F.F. and T.L. performed the differentiation, chromatin immunoprecipitation, co-immunoprecipitation experiments, and immunological assays; F.C.-M. performed the bioinformatic analyses; F.C.-M. A.G.F.-B. G.G.-T. E.M.-C. and E.B. analyzed results; J.R.-U. and E.B. supervised the study; F.C.-M. T.L. and E.B. wrote the manuscript; all authors participated in discussions and interpreting the results. The authors declare no competing interests. The active form of vitamin D, 1,25-dihydroxyvitamin D3, induces a stable tolerogenic phenotype in dendritic cells (DCs). This process involves the vitamin D receptor (VDR), which translocates to the nucleus, binds its cognate genomic sites, and promotes epigenetic and transcriptional remodeling. In this study, we report the occurrence of vitamin D-specific DNA demethylation and transcriptional activation at VDR binding sites associated with the acquisition of tolerogenesis in vitro. Differentiation to tolerogenic DCs associates with activation of the IL-6-JAK-STAT3 pathway. We show that JAK2-mediated STAT3 phosphorylation is specific to vitamin D stimulation. VDR and the phosphorylated form of STAT3 interact with each other to form a complex with methylcytosine dioxygenase TET2. Most importantly, pharmacological inhibition of JAK2 reverts vitamin D-induced tolerogenic properties of DCs. This interplay among VDR, STAT3, and TET2 opens up possibilities for modulating DC immunogenic properties in clinics.

Published

2021

5. The JAK2-STAT pathway epigenetically regulates tolerized genes during the first encounter with bacterial antigens

Author

Damiana Álvarez-Errico, Esteban Ballestar, Antonio Garcia-Gomez, Octavio Morante-Palacios, Francesc Català-Moll, Mónica Martínez-Gallo, Juan Carlos Ruiz-Rodríguez, Adolfo Ruiz-Sanmartín, Ricard Ferrer-Roca, Laura Ciudad, and Clara Lorente-Sorolla

Subjects

chemistry.chemical_compound, biology, Lipopolysaccharide, chemistry, biology.protein, TLR4, STAT protein, JAK-STAT signaling pathway, STAT1, Bacterial antigen, STAT3, STAT5, Cell biology

Abstract

Microbial challenges, such as widespread bacterial infection, induce endotoxin tolerance. This state of hyporesponsiveness to subsequent infections is mainly displayed by monocytes and macrophages. Endotoxin tolerance is generally acquired following a septic episode. In this study, we investigated DNA methylation changes during the acquisition of in vitro tolerance. We identified a set of TET2-mediated demethylation events that are specific to toll-like receptor (TLR) 2 and TLR4 stimulation. Lipopolysaccharide (LPS)-specific demethylation occurs at genomic sites that have low accessibility in quiescent monocytes, concomitantly with the transcriptional activation of many inflammation-related genes, and they are enriched in binding motifs for several signal transducer and activator of transcription (STAT) family members. Indeed, STAT1, STAT3 and STAT5, elements of the JAK2 pathway, are phosphorylated in association with the acquisition of endotoxin tolerance. Inhibition of the JAK2 pathway impairs the activation of tolerized genes on the first encounter with LPS. This is evidence of a crucial role for this pathway in determining the initial response of these genes to bacterial antigens and provides a pharmacological target to prevent exacerbated responses, allowing regulated responses upon subsequent challenges. Finally, we assess the pathological relevance of the JAK2 pathway in monocytes from patients with sepsis.

Published

2020

6. Epigenomics and Transcriptomics of Systemic Sclerosis CD4+ T cells reveal Long Range Dysregulation of Key Inflammatory Pathways mediated by disease-associated Susceptibility Loci

Author

Biola M. Javierre, Elena López-Isac, Laura Ciudad, Javier Martín, Tianlu Li, Alfredo Guillén-Del-Castillo, Eduardo Andrés-León, Lourdes Ortiz, Carmen Pilar Simeón-Aznar, and Esteban Ballestar

Subjects

Genetics, integumentary system, T cell, Inflammation, Biology, Transcriptome, medicine.anatomical_structure, Immune system, CTCF, DNA methylation, medicine, Epigenetics, medicine.symptom, Epigenomics

Abstract

System sclerosis (SSc) is a genetically complex autoimmune disease mediated by the interplay between genetic and epigenetic factors in a multitude of immune cells, with CD4+ T lymphocytes as one of the principle drivers of pathogenesis. In this study, we obtained DNA methylation and expression profiles of CD4+ T cells from 48 SSc patients and 16 healthy controls. Consequently, we identified 9112 and 3929 differentially methylated CpGs positions (DMPs) and differentially expressed genes (DEGs) respectively. These DMPs and DEGs are enriched in functional categories related to inflammation and T cell biology. Furthermore, correlation analysis identified 17,500 possible DMP-DEG interaction pairs within a window of 5 Mb, and utilizing promoter capture Hi-C data, we confirmed that 212 CD4+ T cel specific pairs of DMP-DEG physically interact involving CTCF. Finally, utilizing SSc GWAS data, we identified four important SSc-associated susceptibility loci, TNIP1 (rs3792783), GSDMB (rs9303277), IL12RB1 (rs2305743) and CSK (rs1378942), that physically interact with DMP-DEG pairs cg17239269-ANXA6, cg19458020-CCR7, cg10808810-JUND and cg11062629-ULK3 respectively. Overall, our study reveals a solid link between genetic, epigenetic and transcriptional deregulation in CD4+ T cells of SSc patients, providing a novel integrated view of SSc pathogenic determinants.

Published

2020

7. Vitamin D receptor and STAT3 cooperate to establish TET2-mediated tolerogenesis

Author

Laura Ciudad, Tianlu Li, Francesc Català-Moll, Javier Rodríguez-Ubreva, and Esteban Ballestar

Subjects

DNA demethylation, biology, Chemistry, DNA methylation, Vitamin D and neurology, biology.protein, Phosphorylation, Epigenetics, STAT3, Calcitriol receptor, Transcription factor, Cell biology

Abstract

SUMMARYThe active form of vitamin D, 1,25-dihydroxyvitamin D3 (1,25(OH)2D3), induces stable tolerogenesis in dendritic cells (DCs). This process involves the vitamin D receptor (VDR), which translocates to the nucleus, binds its cognate genomic sites, and promotes epigenetic and transcriptional remodeling. In this study, we investigated the interplay between the VDR and other transcription factors to induce DNA methylation changes that might provide phenotypic stability to the tolerogenic phenotype of DCs. Our study reveals the occurrence of vitamin D-specific DNA demethylation and transcriptional activation at VDR binding sites associated with the acquisition of tolerogenesis. Tolerogenic properties in DCs are acquired together with activation of the IL6-JAK-STAT3 pathway. In fact, VDR directly binds the IL6 gene, and JAK2-mediated STAT3 phosphorylation is specific to vitamin D stimulation. VDR and the phosphorylated form of STAT3 interact with each other and with methylcytosine dioxygenase TET2 following vitamin D treatment. Most importantly, pharmacological inhibition of STAT3 phosphorylation reverts the vitamin-induced tolerogenic properties of DCs. Our results reveal an interplay between VDR and STAT3 leading to the DNA demethylation-dependent induction of tolerogenesis by vitamin D.

Published

2020

8. Inflammatory cytokines and organ dysfunction associate with the aberrant DNA methylome of monocytes in sepsis

Author

Damiana Álvarez-Errico, Antonio Garcia-Gomez, Álvaro García del Campo, Ricard Ferrer-Roca, Laura Ciudad, Victor Toledano, Clara Lorente-Sorolla, Mónica Martínez-Gallo, Eduardo López-Collazo, Francesc Català-Moll, Juan Carlos Ruiz-Rodríguez, Adolfo Ruiz-Sanmartín, Esteban Ballestar, Alejandro Martín-Quirós, Charbel Maroun-Eid, and José Avendaño-Ortiz

Subjects

Male, 0301 basic medicine, lcsh:QH426-470, Multiple Organ Failure, lcsh:Medicine, Endotoxin tolerance, Biology, Monocytes, Proinflammatory cytokine, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Citoquines, Genetics, medicine, Humans, Epigenetics, Molecular Biology, Genetics (clinical), Aged, Inflammation, DNA methylation, Research, lcsh:R, Organ dysfunction, DNA, Methylation, Middle Aged, medicine.disease, Systemic inflammatory response syndrome, lcsh:Genetics, Phenotype, 030104 developmental biology, Insuficiència respiratòria, Case-Control Studies, 030220 oncology & carcinogenesis, Immunology, Molecular Medicine, Cytokines, Female, Inflammation Mediators, medicine.symptom, Respiratory insufficiency, Reprogramming, Signal Transduction

Abstract

Background Sepsis, a life-threatening organ dysfunction caused by a dysregulated systemic immune response to infection, associates with reduced responsiveness to subsequent infections. How such tolerance is acquired is not well understood but is known to involve epigenetic and transcriptional dysregulation. Methods Bead arrays were used to compare global DNA methylation changes in patients with sepsis, non-infectious systemic inflammatory response syndrome, and healthy controls. Bioinformatic analyses were performed to dissect functional reprogramming and signaling pathways related to the acquisition of these specific DNA methylation alterations. Finally, in vitro experiments using human monocytes were performed to test the induction of similar DNA methylation reprogramming. Results Here, we focused on DNA methylation changes associated with sepsis, given their potential role in stabilizing altered phenotypes. Tolerized monocytes from patients with sepsis display changes in their DNA methylomes with respect to those from healthy controls, affecting critical monocyte-related genes. DNA methylation profiles correlate with IL-10 and IL-6 levels, significantly increased in monocytes in sepsis, as well as with the Sequential Organ Failure Assessment score; the observed changes associate with TFs and pathways downstream to toll-like receptors and inflammatory cytokines. In fact, in vitro stimulation of toll-like receptors in monocytes results in similar gains and losses of methylation together with the acquisition of tolerance. Conclusion We have identified a DNA methylation signature associated with sepsis that is downstream to the response of monocytes to inflammatory signals associated with the acquisition of a tolerized phenotype and organic dysfunction.

Published

2019

9. C/EBPa-Mediated Activation of MicroRNAs 34a and 223 Inhibits Lef1 Expression To Achieve Efficient Reprogramming into Macrophages

Author

Esteban Ballestar, Thomas Graf, Laura Ciudad, Javier Rodríguez-Ubreva, Chris van Oevelen, and Maribel Parra

Subjects

Lymphoid Enhancer-Binding Factor 1, PAX5 Transcription Factor, Antigens, CD19, Down-Regulation, Biology, Ikaros Transcription Factor, Mice, Downregulation and upregulation, Animals, Molecular Biology, Transcription factor, B-Lymphocytes, Ccaat-enhancer-binding proteins, Macrophages, Precursor Cells, B-Lymphoid, Transdifferentiation, Articles, Cell Biology, Molecular biology, Up-Regulation, Cell biology, MicroRNAs, Cell Transdifferentiation, CCAAT-Enhancer-Binding Proteins, Trans-Activators, Ectopic expression, Transcription Factors, Lymphoid enhancer-binding factor 1

Abstract

MicroRNAs (miRNAs) exert negative effects on gene expression and influence cell lineage choice during hematopoiesis. C/EBPa-induced pre-B cell-to-macrophage transdifferentiation provides an excellent model to investigate the contribution of miRNAs to hematopoietic cell identity, especially because the two cell types involved fall into separate lymphoid and myeloid branches. In this process, efficient repression of the B cell-specific program is essential to ensure transdifferentation and macrophage function. miRNA profiling revealed that upregulation of miRNAs is highly predominant compared with downregulation and that C/EBPa directly regulates several upregulated miRNAs. We also determined that miRNA 34a (miR-34a) and miR-223 sharply accelerate C/EBPa-mediated transdifferentiation, whereas their depletion delays this process. These two miRNAs affect the transdifferentiation efficiency and activity of macrophages, including their lipopolysaccharide (LPS)-dependent inflammatory response. miR-34a and miR-223 directly target and downregulate the lymphoid transcription factor Lef1, whose ectopic expression delays transdifferentiation to an extent similar to that seen with miR-34a and miR-223 depletion. In addition, ectopic introduction of Lef1 in macrophages causes upregulation of B cell markers, including CD19, Pax5, and Ikzf3. Our report demonstrates the importance of these miRNAs in ensuring the erasure of key B cell transcription factors, such as Lef1, and reinforces the notion of their essential role in fine-tuning the control required for establishing cell identity.

Published

2014

10. Activation-induced cytidine deaminase targets SUV4-20-mediated histone H4K20 trimethylation to class-switch recombination sites

Author

Esteban Ballestar, Javier Rodríguez-Ubreva, Laura Ciudad, Almudena R. Ramiro, Francesc Català-Moll, Alejandro Vaquero, Ganesh Poorani-Subramani, Henar Hernando, Antonio Garcia-Gomez, Arantxa Pérez-García, Virginia C. Rodríguez-Cortez, Javier M. Di Noia, Jose Urquiza, Paloma Martinez-Redondo, Instituto de Salud Carlos III, Unión Europea. Fondo Europeo de Desarrollo Regional (FEDER/ERDF), Canada Research Chairs, and Canadian Institutes of Health Research

Subjects

0301 basic medicine, Lipopolysaccharides, Methyltransferase, DOUBLE-STRAND BREAKS, Hyper-IgM Immunodeficiency Syndrome, Lymphocyte Activation, RECRUIT AID, Epigenesis, Genetic, Histones, Mice, Activation-induced (cytidine) deaminase, Regulation of gene expression, Genetics, B-Lymphocytes, Multidisciplinary, biology, METHYLATION, Cytidine deaminase, REGIONS, Histone, B-CELLS, Medicine, Epigenetics, RNA Polymerase II, Protein Binding, Signal Transduction, Science, Models, Biological, DEMETHYLATION, Article, 03 medical and health sciences, Cell Line, Tumor, Cytidine Deaminase, SOMATIC HYPERMUTATION, Animals, Humans, Binding site, REPAIR, Binding Sites, DNA, Histone-Lysine N-Methyltransferase, Epigenètica, SUPER-ENHANCERS, Immunoglobulin Class Switching, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, Immunoglobulin class switching, Gene Expression Regulation, Immunoglobulin G, Mutation, biology.protein, RNA, HeLa Cells

Abstract

Activation-induced cytidine deaminase (AID) triggers antibody diversification in B cells by catalysing deamination and subsequently mutating immunoglobulin (Ig) genes. Association of AID with RNA Pol II and occurrence of epigenetic changes during Ig gene diversification suggest participation of AID in epigenetic regulation. AID is mutated in hyper-IgM type 2 (HIGM2) syndrome. Here, we investigated the potential role of AID in the acquisition of epigenetic changes. We discovered that AID binding to the IgH locus promotes an increase in H4K20me3. In 293F cells, we demonstrate interaction between co-transfected AID and the three SUV4-20 histone H4K20 methyltransferases, and that SUV4-20H1.2, bound to the IgH switch (S) mu site, is replaced by SUV4-20H2 upon AID binding. Analysis of HIGM2 mutants shows that the AID truncated form W68X is impaired to interact with SUV4-20H1.2 and SUV4-20H2 and is unable to bind and target H4K20me3 to the Smu site. We finally show in mouse primary B cells undergoing class-switch recombination (CSR) that AID deficiency associates with decreased H4K20me3 levels at the Smu site. Our results provide a novel link between SUV4-20 enzymes and CSR and offer a new aspect of the interplay between AID and histone modifications in setting the epigenetic status of CSR sites. This work was supported by grant SAF2014-55942-R from the Instituto de Salud Carlos III, organisms ascribed to the Ministerio de Economia y Competitividad and cofunded by FEDER funds/European Regional Development Fund (ERDF) - a way to build Europe, and the EU FP7 306000 STATegra project. JMDN is supported by a Canada Research Chair tier II. Work by JMDN and SPG was supported by the Canadian Institutes of Health Research, MOP 125991. Sí

Published

2016

11. Pre-B cell to macrophage transdifferentiation without significant promoter DNA methylation changes

Author

David Gomez-Cabrero, Javier Rodríguez-Ubreva, Maribel Parra, Eric M. Kallin, Lars H. Bussmann, Alessandro di Tullio, Esteban Ballestar, Thomas Graf, Jesper Tegnér, and Laura Ciudad

Subjects

Cèl·lules B, Cellular differentiation, ADN, Gene Regulation, Chromatin and Epigenetics, Biology, Epigenesis, Genetic, Histones, Mice, 03 medical and health sciences, 0302 clinical medicine, Epigenetics of physical exercise, CCAAT-Enhancer-Binding Protein-alpha, Genetics, Animals, p300-CBP Transcription Factors, Epigenetics, Promoter Regions, Genetic, Cells, Cultured, 030304 developmental biology, B cells, 0303 health sciences, Macrophages, Precursor Cells, B-Lymphoid, Transdifferentiation, Promoter, DNA, DNA Methylation, Molecular biology, 3. Good health, 030220 oncology & carcinogenesis, Cell Transdifferentiation, DNA methylation, Reprogramming

Abstract

Transcription factor-induced lineage reprogramming or transdifferentiation experiments are essential for understanding the plasticity of differentiated cells. These experiments helped to define the specific role of transcription factors in conferring cell identity and played a key role in the development of the regenerative medicine field. We here investigated the acquisition of DNA methylation changes during C/EBP alpha-induced pre-B cell to macrophage transdifferentiation. Unexpectedly, cell lineage conversion occurred without significant changes in DNA methylation not only in key B cell- and macrophage-specific genes but also throughout the entire set of genes differentially methylated between the two parental cell types. In contrast, active and repressive histone modification marks changed according to the expression levels of these genes. We also demonstrated that C/EBP alpha and RNA Pol II are associated with the methylated promoters of macrophage-specific genes in reprogrammed macrophages without inducing methylation changes. Our findings not only provide insights about the extent and hierarchy of epigenetic events in pre-B cell to macrophage transdifferentiation but also show an important difference to reprogramming towards pluripotency where promoter DNA demethylation plays a pivotal role.

Published

2011

12. Monozygotic twins discordant for common variable immunodeficiency reveal impaired DNA demethylation during naive-to-memory B-cell transition

Author

Virginia C. Rodríguez-Cortez, Lucia del Pino-Molina, Javier Rodríguez-Ubreva, Laura Ciudad, David Gómez-Cabrero, Carlos Company, José M. Urquiza, Jesper Tegnér, Carlos Rodríguez-Gallego, Eduardo López-Granados, and Esteban Ballestar

Subjects

Lymphocyte, Cèl·lules B, ADN, humanos, estudios de casos y controles, General Physics and Astronomy, regulación de la expresión génica, Biology, Article, General Biochemistry, Genetics and Molecular Biology, linfocitos B, 03 medical and health sciences, 0302 clinical medicine, memoria inmunológica, medicine, Immunodeficiency, Humans, Epigenetics, metilación del ADN, Memory B cell, 030304 developmental biology, Regulation of gene expression, Genetics, Immunodeficiència, 0303 health sciences, B cells, B-Lymphocytes, Multidisciplinary, Common variable immunodeficiency, inmunodeficiencia variable común, Twins, Monozygotic, General Chemistry, DNA, DNA Methylation, medicine.disease, 3. Good health, medicine.anatomical_structure, DNA demethylation, Common Variable Immunodeficiency, Gene Expression Regulation, Case-Control Studies, DNA methylation, Immunology, Primary immunodeficiency, Immunologic Memory, 030215 immunology

Abstract

Common variable immunodeficiency (CVID), the most frequent primary immunodeficiency characterized by loss of B-cell function, depends partly on genetic defects, and epigenetic changes are thought to contribute to its aetiology. Here we perform a high-throughput DNA methylation analysis of this disorder using a pair of CVID-discordant MZ twins and show predominant gain of DNA methylation in CVID B cells with respect to those from the healthy sibling in critical B lymphocyte genes, such as PIK3CD, BCL2L1, RPS6KB2, TCF3 and KCNN4. Individual analysis confirms hypermethylation of these genes. Analysis in naive, unswitched and switched memory B cells in a CVID patient cohort shows impaired ability to demethylate and upregulate these genes in transitioning from naive to memory cells in CVID. Our results not only indicate a role for epigenetic alterations in CVID but also identify relevant DNA methylation changes in B cells that could explain the clinical manifestations of CVID individuals., Epigenetic changes are thought to contribute to the aetiology of common variable immunodeficiency (CVID), a disease characterized by loss of B-cell function. Here, by comparing DNA methylation profile in B cells from monozygotic twins discordant for CVID, the authors show a gain of DNA methylation in CVID B cells.

Published

2015

13. NF-κB-direct activation of microRNAs with repressive effects on monocyte-specific genes is critical for osteoclast differentiation

Author

Lorenzo de la Rica, Antonio García-Gómez, Natalia R Comet, Javier Rodríguez-Ubreva, Laura Ciudad, Roser Vento-Tormo, Carlos Company, Damiana Álvarez-Errico, Mireia García, Carmen Gómez-Vaquero, Esteban Ballestar, and Universitat de Barcelona

Subjects

Transcriptional Activation, Micro RNAs, Cellular differentiation, Bones cancer, Osteoclasts, Biology, Artritis reumatoide, Monocytes, Metastasis, Immunomodulation, Genètica mèdica, Downregulation and upregulation, Metàstasi, RNA interference, Osteoclast, Cell diferentiation, medicine, Cluster Analysis, Humans, Position-Specific Scoring Matrices, Gene silencing, Gene Silencing, RNA, Messenger, Epigenetics, Rheumatoid arthritis, Transcription factor, Regulation of gene expression, Binding Sites, Research, Gene Expression Profiling, Medical genetics, NF-kappa B, Càncer d'ossos, Cell Differentiation, Molecular biology, Cell biology, MicroRNAs, medicine.anatomical_structure, Gene Expression Regulation, Organ Specificity, Multigene Family, RNA Interference, Diferenciació cel·lular, Protein Binding

Abstract

Background Monocyte-to-osteoclast conversion is a unique terminal differentiation process that is exacerbated in rheumatoid arthritis and bone metastasis. The mechanisms implicated in upregulating osteoclast-specific genes involve transcription factors, epigenetic regulators and microRNAs (miRNAs). It is less well known how downregulation of osteoclast-inappropriate genes is achieved. Results In this study, analysis of miRNA expression changes in osteoclast differentiation from human primary monocytes revealed the rapid upregulation of two miRNA clusters, miR-212/132 and miR-99b/let-7e/125a. We demonstrate that they negatively target monocyte-specific and immunomodulatory genes like TNFAIP3, IGF1R and IL15. Depletion of these miRNAs inhibits osteoclast differentiation and upregulates their targets. These miRNAs are also upregulated in other inflammatory monocytic differentiation processes. Most importantly, we demonstrate for the first time the direct involvement of Nuclear Factor kappa B (NF-κB) in the regulation of these miRNAs, as well as with their targets, whereby NF-κB p65 binds the promoters of these two miRNA clusters and NF-κB inhibition or depletion results in impaired upregulation of their expression. Conclusions Our results reveal the direct involvement of NF-κB in shutting down certain monocyte-specific genes, including some anti-inflammatory activities, through a miRNA-dependent mechanism for proper osteoclast differentiation. Electronic supplementary material The online version of this article (doi:10.1186/s13059-014-0561-5) contains supplementary material, which is available to authorized users.

Published

2015

14. Long-Range Epigenetic Silencing Associates with Deregulation of Ikaros Targets in Colorectal Cancer Cells

Author

Fatima Al-Shahrour, Xabier Agirre, Felipe Prosper, María José Calasanz, Alfonso Valencia, Marina Corominas, Manel Esteller, Osvaldo Graña, Biola M. Javierre, Jose Roman-Gomez, Esteban Ballestar, Laura Ciudad, Rogelio González-Sarmiento, Javier Rodríguez-Ubreva, and David G. Pisano

Subjects

Cancer Research, Colorectal cancer, Cellular differentiation, Biology, Adenocarcinoma, Ikaros Transcription Factor, medicine, Gene silencing, Humans, Epigenetics, Gene Silencing, Promoter Regions, Genetic, Molecular Biology, Neoplasm Staging, Cancer, Cell Differentiation, DNA Methylation, medicine.disease, HCT116 Cells, Gene Expression Regulation, Neoplastic, Oncology, DNA methylation, Cancer research, Disease Progression, CpG Islands, Colorectal Neoplasms

Abstract

Transcription factors are common targets of epigenetic inactivation in human cancer. Promoter hypermethylation and subsequent silencing of transcription factors can lead to further deregulation of their targets. In this study, we explored the potential epigenetic deregulation in cancer of Ikaros family genes, which code for essential transcription factors in cell differentiation and exhibit genetic defects in hematologic neoplasias. Unexpectedly, our analysis revealed that Ikaros undergoes very specific promoter hypermethylation in colorectal cancer, including in all the cell lines studied and around 64% of primary colorectal adenocarcinomas, with increasing proportions in advanced Duke's stages. Ikaros hypermethylation occurred in the context of a novel long-range epigenetic silencing (LRES) region. Reintroduction of Ikaros in colorectal cancer cells, ChIP-chip analysis, and validation in primary samples led us to identify a number of direct targets that are possibly related with colorectal cancer progression. Our results not only provide the first evidence that LRES can have functional specific effects in cancer but also identify several deregulated Ikaros targets that may contribute to progression in colorectal adenocarcinoma., E. Ballestar is supported by PI081346 grant from the Spanish Ministry of Science and Innovation (MICINN-ISCIII) and 2009SGR184 AGAUR grant (Catalan Government). B.M. Javierre is funded by a BEFI Predoctoral Fellowship from ISCIII, Spain.

Published

2011

15. Conservation of fruitless' role as master regulator of male courtship behaviour from cockroaches to flies

Author

Elke Clynen, Xavier Bellés, Maria-Dolors Piulachs, Laura Ciudad, Ministerio de Educación y Ciencia (España), Generalitat de Catalunya, European Commission, Consejo Superior de Investigaciones Científicas (España), and Research Foundation - Flanders

Subjects

Male, media_common.quotation_subject, RNA Splicing, Cockroaches, Nerve Tissue Proteins, Fruitless, Courtship, Sexual Behavior, Animal, biology.animal, Genetics, Melanogaster, Animals, Drosophila Proteins, Drosophila, media_common, Cockroach, German cockroach, Courtship behaviour, biology, Courtship display, Base Sequence, fungi, Zinc Fingers, biology.organism_classification, Biological Evolution, Blattella germanica, Drosophila melanogaster, RNAi, fruitless, RNA Interference, Insect, Developmental Biology, Transcription Factors

Abstract

In Drosophila melanogaster, male courtship behaviour is regulated by the fruitless gene. In D. melanogaster, fruitless encodes a set of putative transcription factors that are sex-specifically spliced. Male-specific variants are necessary and sufficient to elicit male courtship behaviour. Fruitless sequences have been reported in other insect species, but there are no data available on their functional role. In the present work, we cloned and sequenced fruitless in males of the German cockroach, Blattella germanica, and we studied its expression in male brain and testes. B. germanica fruitless encodes a 350-amino acid protein with BTB and Zinc finger domains typical of fruitless sequences. Upon RNAi-mediated knockdown of fruitless in B. germanica, males no longer exhibit courtship behaviour, thus implying that fruitless is necessary for male sexual behaviour in our cockroach model. This suggests that the role of fruitless as master regulator of male sexual behaviour has been conserved along insect evolution, at least from cockroaches to flies., Financial support from the Ministry of Education and Science, Spain (projects BFU2008-00484 to M-D. Piulachs and CGL2008-03517/BOS to X. Bellés), Generalitat de Catalunya (2005 SGR 00053) is gratefully acknowledged. L. Ciudad received a pre-doctoral research grant (I3P) from CSIC, and E. Clynen received a travel grant from the Fund for Scientific Research (FWO)-Flanders (Belgium) to work in the Institute of Evolutionary Biology in Barcelona. Thanks are also due to Elena Torres, who received a JAE-intro (CSIC) grant, for helping in the experimental work.

Published

2010

16. Immunomodulatory effect of 5-azacytidine (5-azaC): potential role in the transplantation setting

Author

Teresa Caballero-Velázquez, Jesús F. San Miguel, Laura Ciudad, José A. Pérez-Simón, Carlos Santamaría, Esteban Ballestar, Luis Ignacio Sánchez-Abarca, Consuelo del Cañizo, Soraya Carrancio, Juan Luis García, Belén Blanco, Carmen Herrero-Sánchez, Teresa Flores, Pilar Hernandez-Campo, Francisco Gonzalez, and Silvia Gutierrez-Cosio

Subjects

Male, Cell Survival, Immunology, Azacitidine, DNA Methyltransferase Inhibitor, Graft vs Host Disease, Biology, Lymphocyte Activation, Biochemistry, T-Lymphocytes, Regulatory, Proinflammatory cytokine, Mice, medicine, Animals, Humans, Immunologic Factors, Transplantation, Homologous, Lymphocyte Count, Promoter Regions, Genetic, Bone Marrow Transplantation, Cell Proliferation, Gene Expression Profiling, Cell Cycle, Immunity, FOXP3, Forkhead Transcription Factors, Cell Biology, Hematology, Cell cycle, DNA Methylation, Survival Analysis, Transplantation, Gene Expression Regulation, Cancer research, Tumor necrosis factor alpha, Female, GADD45B, Spleen, medicine.drug

Abstract

Cytokine genes are targets of multiple epigenetic mechanisms in T lymphocytes. 5-azacytidine (5-azaC) is a nucleoside-based DNA methyltransferase inhibitor that induces demethylation and gene reactivation. In the current study, we analyzed the effect of 5-azaC in T-cell function and observed that 5-azaC inhibits T-cell proliferation and activation, blocking cell cycle in the G0 to G1 phase and decreasing the production of proinflammatory cytokines such as tumor necrosis factor-α and interferon-γ. This effect was not attributable to a proapoptotic effect of the drug but to the down-regulation of genes involved in T-cell cycle progression and activation such as CCNG2, MTCP1, CD58, and ADK and up-regulation of genes that induce cell-growth arrest, such as DCUN1D2, U2AF2, GADD45B, or p53. A longer exposure to the drug leads to demethylation of FOXP3 promoter, overexpression of FOXP3, and expansion of regulatory T cells. Finally, the administration of 5-azaC after transplantation prevented the development of graft-versus-host disease, leading to a significant increase in survival in a fully mismatched bone marrow transplantation mouse model. In conclusion, the current study shows the effect of 5-azaC in T lymphocytes and illustrates its role in the allogeneic transplantation setting as an immunomodulatory drug, describing new pathways that must be explored to prevent graft-versus-host disease.

Published

2009

17. Effect of Demethylating Agents (5-Azacytidine/5-AzaC) On the Immune Response

Author

Consuelo del Cañizo, Laura Ciudad, Belén Blanco, Silvia Gutiérrez Cosío, Luis Ignacio Sánchez Abarca, Teresa Caballero Velázquez, Soraya Carrancio, Carlos Santamaría, Carmen Sánchez, Jesús F. San Miguel, Esteban Ballestar, and Jose Antonio Pérez Simón

Subjects

Immunology, Azacitidine, GATA3, FOXP3, Promoter, Cell Biology, Hematology, Methylation, Biology, Biochemistry, Demethylating agent, chemistry.chemical_compound, Immune system, chemistry, medicine, Epigenetics, medicine.drug

Abstract

Abstract 2771 Introduction: We have previously shown that 5-azaC inhibits T-cells proliferation and favours the development of Tregs which decreases the risk of GVHD after allogeneic transplantation. This is at least in part due to the effect of the drug on the expression of genes such as FOXP3. Nevertheless, considering the unspecific effect of 5-azaC, it could also favour the overexpression of other genes related to the regulation of the immune response such as TBET, GATA3, IFNg or IL-2, which in turn would favour the development of a Th1, Th2 or Th17 polarization instead of a Treg expansion. In the current study we have evaluated the effect of 5-azaC on these genes in order to know the mechanisms involved in the effect of the drug on the immune response. Methods: We analyzed TBET, GATA3, FOXP3, IFNg and IL-2 mRNA expression of T lymphocytes by RT-PCR after exposure to 1mM 5-azaC during eleven days of culture. These T cells were cultured in medium alone or stimulated with plate-bound anti-CD3 (5 mg/ml) plus soluble anti-CD28 (2.5 mg/ml). Furthermore, we analyzed the methylation status of the promoters of these genes before and after 5-azaC treatment. Results: The expression of TBET, GATA3 and RORγ is not significantly affected by the exposure to the drug whereas the expression of FOXP3 significantly increases along the culture. Regarding IFNg and IL-2 expression no increased expression was observed after exposure to the drug at different time-points along the 11 days of culture. Upon analyzing the mathylation status of the promoter of these genes, we observed that in steady state the promoter of TBET and GATA is demethylated, which is in contrast to FOXP3 promoter. For this reason, the exposure to the drug decreases the methylation status of the promoter of FOXP3 while there is no effect on the promoters of TBET or RORg, thus justifying the absence of effect on the expression of these genes. By contrat, the promoter of both IFNg and IL-2 is methylated prior to the exposure to 5-azaC and it is demethylated after exposure to the drug, which is in contrast to the absence of increased expression of these genes. Accordingly, other mechanisms in addition to the epigenetic regulation of the promoter of IFNg and IL-2 are responsible for their expression in this model. Conclusions: In the current study we show by the first time the effect of 5-azaC on the promoters of genes which regulate the immune response. While no effect was observed for TBET, and GATA3 5-azaC induces a strong demethylation in the promoter of IFN or IL-2. In spite of this effect there is no increase in their expression which could be due to the overexpression of FOXP3 or to additional mechanisms involved in their regulation which are currently being evaluated. Disclosures: Cañizo: Celgene: Membership on an entity's Board of Directors or advisory committees. San Miguel:Celgene: Membership on an entity's Board of Directors or advisory committees; Novartis: Membership on an entity's Board of Directors or advisory committees; Jangssen-cilag: Membership on an entity's Board of Directors or advisory committees; millennium: Membership on an entity's Board of Directors or advisory committees. Off Label Use: The drug used in this study is the demethylating agent 5-azacytidine (5-azaC) and the purpose is the inhibition of graft versus host disease.

Published

2010

18. Structural and RNAi characterization of the German cockroach lipophorin receptor, and the evolutionary relationships of lipoprotein receptors

Author

Xavier Bellés, Maria-Dolors Piulachs, and Laura Ciudad

Subjects

Gene isoform, Very low-density lipoprotein, lcsh:QH426-470, Gene Expression, Receptors, Cytoplasmic and Nuclear, Cockroaches, Ovary, Biology, Evolution, Molecular, chemistry.chemical_compound, medicine, Animals, lcsh:QH573-671, Receptor, Molecular Biology, Phylogeny, Sequence Homology, Amino Acid, lcsh:Cytology, lcsh:Genetics, medicine.anatomical_structure, chemistry, Biochemistry, Low-density lipoprotein, Juvenile hormone, LDL receptor, Insect Proteins, Female, RNA Interference, Vitellogenesis, Research Article

Abstract

This article is available from: http://www.biomedcentral.com/1471-2199/8/53, [Background] Lipophorin receptors (LpRs) have been described in a number of insects, but functional studies have been reported only in locusts and mosquitoes. The aim of the present work was to characterize the LpR of the cockroach Blattella germanica, not only molecularly but also functionally using RNAi techniques, and to place LpRs in a phylogenetical context among lipoprotein receptors., [Results] We cloned a putative LpR from B. germanica (BgLpR) using RT-PCR methods. Two isoforms of BgLpR that differ from each other by an insertion/deletion of 24 amino acids were obtained from the fat body and the ovary. A phylogenetical analysis of lipoprotein receptors showed that BgLpR grouped with other sequences annotated as LpR in a cluster placed as a sister group of vertebrate low density lipoprotein receptors (LDLR) + lipoprotein receptor-related proteins 8 (LPR8) + vitellogenin receptors (VgR) + very low density lipoprotein receptors (VLDLR). The two BgLpR isoforms are expressed in different adult female tissues (fat body, ovary, brain, midgut, muscle) and in embryos. In ovaries and fat body, the two isoforms are similarly expressed during the first gonadotrophic cycle. mRNA levels in the fat body increase in parallel to vitellogenesis, whereas they decrease in the ovaries. BgLpR protein levels increase in parallel to vitellogenesis in both organs. Treatment with juvenile hormone increases BgLpR protein. RNAi experiments show that females with lower BgLpR expression have less lipophorin in the growing oocytes with respect to controls., [Conclusion] The two isoforms of BgLpR are structurally similar to other LpRs. Phylogenetical analyses show that LpRs and the group formed by vertebrate LDLR + LPR8 + VgR + VLDLR, diverged from a common ancestor and diversified in parallel. The different expression patterns in the fat body and the ovary, comparing mRNA and protein, indicate that the corresponding mechanisms regulating BgLpR expression are different. Experiments with JH III suggest that such a hormone regulates the expression of BgLpR posttranscriptionally. RNAi experiments indicate that BgLpR is a functional lipophorin receptor., Financial support from the Ministry of Education and Science, Spain (projects BOS2002-03359, BFU2005-00264, AGL2002-01169, AGL2005- 00773) and the Generalitat de Catalunya (2001 SGR 003245) is gratefully acknowledged. L.C. is recipient of pre-doctoral research grants (I3P) from CSIC. We thank Prof. Coby Schal (North Carolina State University) for generous gifts of anti-lipophorin antibody.

Published

2007

19. Epstein–Barr virus-mediated transformation of B cells induces global chromatin changes independent to the acquisition of proliferation

Author

Abul B. M. M. K. Islam, Axel Imhof, Esteban Ballestar, Javier Rodríguez-Ubreva, Laura Ciudad, Claire Shannon-Lowe, Ignasi Forné, and Henar Hernando

Subjects

Herpesvirus 4, Human, Herpesviruses, Heterochromatin, Cèl·lules B, Gene Regulation, Chromatin and Epigenetics, medicine.disease_cause, Histones, Transformation, Genetic, Genetics, medicine, Humans, Constitutive heterochromatin, Cell Proliferation, B-Lymphocytes, B cells, CD40, biology, Cell growth, Herpesvirus, Epstein–Barr virus, Molecular biology, Chromatin, Histone, biology.protein, Deoxyribonuclease I

Abstract

Epstein-Barr virus (EBV) infects and transforms human primary B cells inducing indefinite proliferation. To investigate the potential participation of chromatin mechanisms during the EBV-mediated transformation of resting B cells we performed an analysis of global changes in histone modifications. We observed a remarkable decrease and redistribution of heterochromatin marks including H4K20me3, H3K27me3 and H3K9me3. Loss of H4K20me3 and H3K9me3 occurred at constitutive heterochromatin repeats. For H3K27me3 and H3K9me3, comparison of ChIP-seq data revealed a decrease in these marks in thousands of genes, including clusters of HOX and ZNF genes, respectively. Moreover, DNase-seq data comparison between resting and EBV-transformed B cells revealed increased endonuclease accessibility in thousands of genomic sites. We observed that both loss of H3K27me3 and increased accessibility are associated with transcriptional activation. These changes only occurred in B cells transformed with EBV and not in those stimulated to proliferate with CD40L/IL-4, despite their similarities in the cell pathways involved and proliferation rates. In fact, B cells infected with EBNA-2 deficient EBV, which have much lower proliferation rates, displayed similar decreases for heterochromatic histone marks. Our study describes a novel phenomenon related to transformation of B cells, and highlights its independence of the pure acquisition of proliferation.