Your search keyword '"Pisano, David G."' showing total 14 results

1. Calcitriol inhibits the protumoral properties of colorectal cancer-associated fibroblasts and high VDR expression in these cells predicts a better patient clinical outcome

Author

Ferrer-Mayorga, Gemma, Gómez-López, Gonzalo, Peña, Cristina, Pisano, David G., Cantero, Ramón, Rojo, Federico, Muñoz Terol, Alberto, Larriba, María Jesús, Ferrer-Mayorga, Gemma, Gómez-López, Gonzalo, Peña, Cristina, Pisano, David G., Cantero, Ramón, Rojo, Federico, Muñoz Terol, Alberto, and Larriba, María Jesús

Published

2018

2. The EMBRACE web service collection

Author

Pettifer, Steve, Ison, Jon, Kalaš, Mat�š, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fern�ndez, Jos� M., Rodriguez, Jose M., Partners, INB, Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, Vriend, Gert, Pettifer, Steve, Ison, Jon, Kalaš, Mat�š, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fern�ndez, Jos� M., Rodriguez, Jose M., Partners, INB, Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, and Vriend, Gert

Abstract

The EMBRACE (European Model for Bioinformatics Research and Community Education) web service collection is the culmination of a 5-year project that set out to investigate issues involved in developing and deploying web services for use in the life sciences. The project concluded that in order for web services to achieve widespread adoption, standards must be defined for the choice of web service technology, for semantically annotating both service function and the data exchanged, and a mechanism for discovering services must be provided. Building on this, the project developed: EDAM, an ontology for describing life science web services; BioXSD, a schema for exchanging data between services; and a centralized registry (http://www.embraceregistry.net) that collects together around 1000 services developed by the consortium partners. This article presents the current status of the collection and its associated recommendations and standards definitions

Published

2017

3. Exome sequencing reveals novel and recurrent mutations with clinical impact in blastic plasmacytoid dendritic cell neoplasm

Author

Menezes, J., Gómez-López, Gonzalo, Hernández, Jesús M., Pisano, David G., Cigudosa, Juan C., Menezes, J., Gómez-López, Gonzalo, Hernández, Jesús M., Pisano, David G., and Cigudosa, Juan C.

Abstract

Blastic plasmacytoid dendritic cell neoplasm (BPDCN) is a very rare disease that currently lacks genomic and genetic biomarkers to assist in its clinical management. We performed whole-exome sequencing (WES) of three BPDCN cases. Based on these data, we designed a resequencing approach to identify mutations in 38 selected genes in 25 BPDCN samples. WES revealed 37-99 deleterious gene mutations per exome with no common affected genes between patients, but with clear overlap in terms of molecular and disease pathways (hematological and dermatological disease). We identified for the first time deleterious mutations in IKZF3, HOXB9, UBE2G2 and ZEB2 in human leukemia. Target sequencing identified 29 recurring genes, ranging in prevalence from 36% for previously known genes, such as TET2, to 12-16% for newly identified genes, such as IKZF3 or ZEB2. Half of the tumors had mutations affecting either the DNA methylation or chromatin remodeling pathways. The clinical analysis revealed that patients with mutations in DNA methylation pathway had a significantly reduced overall survival (P=0.047). We provide the first mutational profiling of BPDCN. The data support the current WHO classification of the disease as a myeloid disorder and provide a biological rationale for the incorporation of epigenetic therapies for its treatment.

Published

2014

4. RAB7 Controls Melanoma Progression by Exploiting a Lineage-Specific Wiring of the Endolysosomal Pathway

Author

Ministerio de Ciencia e Innovación (España), Ministerio de Economía y Competitividad (España), National Institutes of Health (US), Melanoma Research Alliance (US), Ministerio de Sanidad (España), Fundación Mutua Madrileña, Fundación Científica Asociación Española Contra el Cáncer, American Cancer Society, Alonso-Curbelo, Direna, Riveiro-Falkenbach, Erica, Pérez-Guijarro, Eva, Cifdaloz, Metehan, Karras, Panagiotis, Osterloh, Lisa, Megías, Diego, Cañón, Estela, Calvo, Tonantzin G., Olmeda, David, Gómez-López, Gonzalo, Graña, Osvaldo, Sánchez-Arévalo Lobo, Víctor J., Pisano, David G., Wang, Hao-Wei, Ortiz-Romero, Pablo, Tormo, Damià, Hoek, Keith, Rodríguez-Peralto, José L., Joyce, Johanna A., Soengas, María S., Ministerio de Ciencia e Innovación (España), Ministerio de Economía y Competitividad (España), National Institutes of Health (US), Melanoma Research Alliance (US), Ministerio de Sanidad (España), Fundación Mutua Madrileña, Fundación Científica Asociación Española Contra el Cáncer, American Cancer Society, Alonso-Curbelo, Direna, Riveiro-Falkenbach, Erica, Pérez-Guijarro, Eva, Cifdaloz, Metehan, Karras, Panagiotis, Osterloh, Lisa, Megías, Diego, Cañón, Estela, Calvo, Tonantzin G., Olmeda, David, Gómez-López, Gonzalo, Graña, Osvaldo, Sánchez-Arévalo Lobo, Víctor J., Pisano, David G., Wang, Hao-Wei, Ortiz-Romero, Pablo, Tormo, Damià, Hoek, Keith, Rodríguez-Peralto, José L., Joyce, Johanna A., and Soengas, María S.

Abstract

Although common cancer hallmarks are well established, lineage-restricted oncogenes remain less understood. Here, we report an inherent dependency of melanoma cells on the small GTPase RAB7, identified within a lysosomal gene cluster that distinguishes this malignancy from over 35 tumor types. Analyses in human cells, clinical specimens, and mouse models demonstrated that RAB7 is an early-induced melanoma driver whose levels can be tuned to favor tumor invasion, ultimately defining metastatic risk. Importantly, RAB7 levels and function were independent of MITF, the best-characterized melanocyte lineage-specific transcription factor. Instead, we describe the neuroectodermal master modulator SOX10 and the oncogene MYC as RAB7 regulators. These results reveal a unique wiring of the lysosomal pathway that melanomas exploit to foster tumor progression.

Published

2014

5. Distinct DNA methylomes of newborns and centenarians

Author

Heyn, Holger, Li, Ning, Ferreira, Humberto J., Moran, Sebastian, Pisano, David G., Gomez, Antonio, Diez, Javier, Sanchez-Mut, Jose V., Setien, Fernando, Carmona, F. Javier, Puca, Annibale A., Sayols, Sergi, Pujana, Miguel A., Serra-Musach, Jordi, Iglesias-Platas, Isabel, Formiga, Francesc, Fernandez, Agustin F., Fraga, Mario F., Heath, Simon C., Valencia, Alfonso, Gut, Ivo G., Wang, Jun, Esteller, Manel, Heyn, Holger, Li, Ning, Ferreira, Humberto J., Moran, Sebastian, Pisano, David G., Gomez, Antonio, Diez, Javier, Sanchez-Mut, Jose V., Setien, Fernando, Carmona, F. Javier, Puca, Annibale A., Sayols, Sergi, Pujana, Miguel A., Serra-Musach, Jordi, Iglesias-Platas, Isabel, Formiga, Francesc, Fernandez, Agustin F., Fraga, Mario F., Heath, Simon C., Valencia, Alfonso, Gut, Ivo G., Wang, Jun, and Esteller, Manel

Abstract

Human aging cannot be fully understood in terms of the constrained genetic setting. Epigenetic drift is an alternative means of explaining age-associated alterations. To address this issue, we performed whole-genome bisulfite sequencing (WGBS) of newborn and centenarian genomes. The centenarian DNA had a lower DNA methylation content and a reduced correlation in the methylation status of neighboring cytosine--phosphate--guanine (CpGs) throughout the genome in comparison with the more homogeneously methylated newborn DNA. The more hypomethylated CpGs observed in the centenarian DNA compared with the neonate covered all genomic compartments, such as promoters, exonic, intronic, and intergenic regions. For regulatory regions, the most hypomethylated sequences in the centenarian DNA were present mainly at CpG-poor promoters and in tissue-specific genes, whereas a greater level of DNA methylation was observed in CpG island promoters. We extended the study to a larger cohort of newborn and nonagenarian samples using a 450,000 CpG-site DNA methylation microarray that reinforced the observation of more hypomethylated DNA sequences in the advanced age group. WGBS and 450,000 analyses of middle-age individuals demonstrated DNA methylomes in the crossroad between the newborn and the nonagenarian/centenarian groups. Our study constitutes a unique DNA methylation analysis of the extreme points of human life at a single-nucleotide resolution level.

Published

2012

6. Genome-wide analysis of Pax8 binding provides new insights into thyroid functions

Author

Comunidad de Madrid, Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Ruiz-Llorente, Sergio, Carrillo Santa de Pau, Enrique, Sastre-Perona, Ana, Montero-Conde, Cristina, Gómez-López, Gonzalo, Fagin, James A., Valencia, Alfonso, Pisano, David G., Santisteban, Pilar, Comunidad de Madrid, Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Ruiz-Llorente, Sergio, Carrillo Santa de Pau, Enrique, Sastre-Perona, Ana, Montero-Conde, Cristina, Gómez-López, Gonzalo, Fagin, James A., Valencia, Alfonso, Pisano, David G., and Santisteban, Pilar

Abstract

[Background]: The transcription factor Pax8 is essential for the differentiation of thyroid cells. However, there are few data on genes transcriptionally regulated by Pax8 other than thyroid-related genes. To better understand the role of Pax8 in the biology of thyroid cells, we obtained transcriptional profiles of Pax8-silenced PCCl3 thyroid cells using whole genome expression arrays and integrated these signals with global cis-regulatory sequencing studies performed by ChIP-Seq analysis [Results]: Exhaustive analysis of Pax8 immunoprecipitated peaks demonstrated preferential binding to intragenic regions and CpG-enriched islands, which suggests a role of Pax8 in transcriptional regulation of orphan CpG regions. In addition, ChIP-Seq allowed us to identify Pax8 partners, including proteins involved in tertiary DNA structure (CTCF) and chromatin remodeling (Sp1), and these direct transcriptional interactions were confirmed in vivo. Moreover, both factors modulate Pax8-dependent transcriptional activation of the sodium iodide symporter (Nis) gene promoter. We ultimately combined putative and novel Pax8 binding sites with actual target gene expression regulation to define Pax8-dependent genes. Functional classification suggests that Pax8-regulated genes may be directly involved in important processes of thyroid cell function such as cell proliferation and differentiation, apoptosis, cell polarity, motion and adhesion, and a plethora of DNA/protein-related processes. [Conclusion]: Our study provides novel insights into the role of Pax8 in thyroid biology, exerted through transcriptional regulation of important genes involved in critical thyrocyte processes. In addition, we found new transcriptional partners of Pax8, which functionally cooperate with Pax8 in the regulation of thyroid gene transcription. Besides, our data demonstrate preferential location of Pax8 in non-promoter CpG regions. These data point to an orphan CpG island-mediated mechanism that represents a no

Published

2012

7. Distinct DNA methylomes of newborns and centenarians

Author

Heyn, Holger, Li, Ning, Ferreira, Humberto J., Moran, Sebastian, Pisano, David G., Gomez, Antonio, Diez, Javier, Sanchez-Mut, Jose V., Setien, Fernando, Carmona, F. Javier, Puca, Annibale A., Sayols, Sergi, Pujana, Miguel A., Serra-Musach, Jordi, Iglesias-Platas, Isabel, Formiga, Francesc, Fernandez, Agustin F., Fraga, Mario F., Heath, Simon C., Valencia, Alfonso, Gut, Ivo G., Wang, Jun, Esteller, Manel, Heyn, Holger, Li, Ning, Ferreira, Humberto J., Moran, Sebastian, Pisano, David G., Gomez, Antonio, Diez, Javier, Sanchez-Mut, Jose V., Setien, Fernando, Carmona, F. Javier, Puca, Annibale A., Sayols, Sergi, Pujana, Miguel A., Serra-Musach, Jordi, Iglesias-Platas, Isabel, Formiga, Francesc, Fernandez, Agustin F., Fraga, Mario F., Heath, Simon C., Valencia, Alfonso, Gut, Ivo G., Wang, Jun, and Esteller, Manel

Abstract

Human aging cannot be fully understood in terms of the constrained genetic setting. Epigenetic drift is an alternative means of explaining age-associated alterations. To address this issue, we performed whole-genome bisulfite sequencing (WGBS) of newborn and centenarian genomes. The centenarian DNA had a lower DNA methylation content and a reduced correlation in the methylation status of neighboring cytosine--phosphate--guanine (CpGs) throughout the genome in comparison with the more homogeneously methylated newborn DNA. The more hypomethylated CpGs observed in the centenarian DNA compared with the neonate covered all genomic compartments, such as promoters, exonic, intronic, and intergenic regions. For regulatory regions, the most hypomethylated sequences in the centenarian DNA were present mainly at CpG-poor promoters and in tissue-specific genes, whereas a greater level of DNA methylation was observed in CpG island promoters. We extended the study to a larger cohort of newborn and nonagenarian samples using a 450,000 CpG-site DNA methylation microarray that reinforced the observation of more hypomethylated DNA sequences in the advanced age group. WGBS and 450,000 analyses of middle-age individuals demonstrated DNA methylomes in the crossroad between the newborn and the nonagenarian/centenarian groups. Our study constitutes a unique DNA methylation analysis of the extreme points of human life at a single-nucleotide resolution level.

Published

2012

8. Combinatorial effects of microRNAs to suppress the Myc oncogenic pathway

Author

Association for International Cancer Research, Fundación Ramón Areces, Fundación Mutua Madrileña, Ministerio de Economía y Competitividad (España), Centro de Investigación Biomédica en Red Enfermedades Raras (España), Fundación Genoma España, Comunidad de Madrid, European Commission, Bueno, María J., Gómez de Cedrón, Marta, Gómez-López, Gonzalo, Pérez de Castro, Ignacio, Lisio, Lorena di, Montes, Santiago, Martínez, Nerea, Guerrero, Manuel, Sánchez-Martínez, Ruth, Santos, Javier, Pisano, David G., Piris, Miguel Ángel, Fernández-Piqueras, José, Malumbres, Marcos, Association for International Cancer Research, Fundación Ramón Areces, Fundación Mutua Madrileña, Ministerio de Economía y Competitividad (España), Centro de Investigación Biomédica en Red Enfermedades Raras (España), Fundación Genoma España, Comunidad de Madrid, European Commission, Bueno, María J., Gómez de Cedrón, Marta, Gómez-López, Gonzalo, Pérez de Castro, Ignacio, Lisio, Lorena di, Montes, Santiago, Martínez, Nerea, Guerrero, Manuel, Sánchez-Martínez, Ruth, Santos, Javier, Pisano, David G., Piris, Miguel Ángel, Fernández-Piqueras, José, and Malumbres, Marcos

Abstract

Many mammalian transcripts contain target sites for multiple miRNAs although it is not clear to what extent miRNAs may coordinately regulate single genes. We have mapped the interactions between downregulated miRNAs and overexpressed target protein-coding genes in murine and human lymphomas. Myc, one of the hallmark oncogenes in these lymphomas, stands out as the upregulated gene with the highest number of genetic interactions with downregulated miRNAs in mouse lymphomas. The regulation of Myc by several of these miRNAs is confirmed by cellular and reporter assays. The same approach indentifies MYC and multiple Myc targets as a preferential target of downregulated miRNAs in human Burkitt's lymphoma, a pathology characterized by translocated MYC oncogenes. These results indicate that several miRNAs must be coordinately downregulated in order to enhance critical oncogenes such as Myc. Some of these Myc-targeting miRNAs are repressed by Myc, suggesting that these tumors are a consequence of the unbalanced activity of Myc versus miRNAs.

Published

2011

9. Cdc14b regulates mammalian RNA polymerase II and represses cell cycle transcription

Author

Guillamot, María, Manchado, Eusebio, Chiesa, Massimo, Gómez-López, Gonzalo, Pisano, David G., Sacristán, María P., Malumbres, Marcos, Guillamot, María, Manchado, Eusebio, Chiesa, Massimo, Gómez-López, Gonzalo, Pisano, David G., Sacristán, María P., and Malumbres, Marcos

Abstract

Cdc14 is an essential phosphatase in yeast but its role in the mammalian cell cycle remains obscure. We report here that Cdc14b-knockout cells display unscheduled induction of multiple cell cycle regulators resulting in early entry into DNA replication and mitosis from quiescence. Cdc14b dephosphorylates Ser5 at the C-terminal domain (CTD) of RNA polymerase II, a major substrate of cyclin-dependent kinases. Lack of Cdc14b results in increased CTD-Ser5 phosphorylation, epigenetic modifications that mark active chromatin, and transcriptional induction of cell cycle regulators. These data suggest a function for mammalian Cdc14 phosphatases in the control of transcription during the cell cycle.

Published

2011

10. The EMBRACE web service collection

Author

Pettifer, Steve, Ison, Jon, Kalas, Matus, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fernandez, Jose M., Rodriguez, Jose M., Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, Vriend, Gert, Pettifer, Steve, Ison, Jon, Kalas, Matus, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fernandez, Jose M., Rodriguez, Jose M., Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, and Vriend, Gert

Abstract

The EMBRACE ( European Model for Bioinformatics Research and Community Education) web service collection is the culmination of a 5-year project that set out to investigate issues involved in developing and deploying web services for use in the life sciences. The project concluded that in order for web services to achieve widespread adoption, standards must be defined for the choice of web service technology, for semantically annotating both service function and the data exchanged, and a mechanism for discovering services must be provided. Building on this, the project developed: EDAM, an ontology for describing life science web services; BioXSD, a schema for exchanging data between services; and a centralized registry (http://www.embraceregistry.net) that collects together around 1000 services developed by the consortium partners. This article presents the current status of the collection and its associated recommendations and standards definitions.

Published

2010

11. CARGO: a web portal to integrate customized biological information

Author

Ministerio de Economía y Competitividad (España), European Commission, Biomedical Research Institute of Vigo, Cases, Ildefonso, Pisano, David G., Andrés-León, Eduardo, Carro, Ángel, Fernández, José M., Gómez-López, Gonzalo, Rodríguez, J. M., Vera, Jaime F., Valencia, Alfonso, Rojas Mendoza, Ana M., Ministerio de Economía y Competitividad (España), European Commission, Biomedical Research Institute of Vigo, Cases, Ildefonso, Pisano, David G., Andrés-León, Eduardo, Carro, Ángel, Fernández, José M., Gómez-López, Gonzalo, Rodríguez, J. M., Vera, Jaime F., Valencia, Alfonso, and Rojas Mendoza, Ana M.

Abstract

There is a huge quantity of information generated in Life Sciences, and it is dispersed in many databases and repositories. Despite the broad availability of the information, there is a great demand for methods that are able to look for, gather and display distributed data in a standardized and friendly way. CARGO (Cancer And Related Genes Online) is a configurable biological web portal designed as a tool to facilitate, integrate and visualize results from Internet resources, independently of their native format or access method. Through the use of small agents, called widgets, supported by a Rich Internet Application (RIA) paradigm based on AJAX, CARGO provides pieces of minimal, relevant and descriptive biological information. The tool is designed to be used by experimental biologists with no training in bioinformatics. In the current state, the system presents a list of human cancer genes. Available at http://cargo.bioinfo.cnio.es

Published

2007

12. Pointers to understand cancer components: developing a system knowledge portal

Author

Rojas Mendoza, Ana M., Juan, David de, Cases, Ildefonso, Pisano, David G., Valencia, Alfonso, Rojas Mendoza, Ana M., Juan, David de, Cases, Ildefonso, Pisano, David G., and Valencia, Alfonso

Published

2006

13. Systems for the analyses of potential cancer target gene-lists

Author

Rojas Mendoza, Ana M., Rodríguez, J. M., Pisano, David G., Gómez-López, Gonzalo, Fernández-Vera, Jaime, Juan, David de, Cases, Ildefonso, Valencia, Alfonso, Rojas Mendoza, Ana M., Rodríguez, J. M., Pisano, David G., Gómez-López, Gonzalo, Fernández-Vera, Jaime, Juan, David de, Cases, Ildefonso, and Valencia, Alfonso

Published

2006

14. The EMBRACE web service collection

Author

Pettifer, Steve, Ison, Jon, Kalaš, Mat�š, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fern�ndez, Jos� M., Rodriguez, Jose M., Partners, INB, Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, Vriend, Gert, Pettifer, Steve, Ison, Jon, Kalaš, Mat�š, Thorne, Dave, McDermott, Philip, Jonassen, Inge, Liaquat, Ali, Fern�ndez, Jos� M., Rodriguez, Jose M., Partners, INB, Pisano, David G., Blanchet, Christophe, Uludag, Mahmut, Rice, Peter, Bartaseviciute, Edita, Rapacki, Kristoffer, Hekkelman, Maarten, Sand, Olivier, Stockinger, Heinz, Clegg, Andrew B., Bongcam-Rudloff, Erik, Salzemann, Jean, Breton, Vincent, Attwood, Teresa K., Cameron, Graham, and Vriend, Gert

Abstract

The EMBRACE (European Model for Bioinformatics Research and Community Education) web service collection is the culmination of a 5-year project that set out to investigate issues involved in developing and deploying web services for use in the life sciences. The project concluded that in order for web services to achieve widespread adoption, standards must be defined for the choice of web service technology, for semantically annotating both service function and the data exchanged, and a mechanism for discovering services must be provided. Building on this, the project developed: EDAM, an ontology for describing life science web services; BioXSD, a schema for exchanging data between services; and a centralized registry (http://www.embraceregistry.net) that collects together around 1000 services developed by the consortium partners. This article presents the current status of the collection and its associated recommendations and standards definitions