Generation of biological association networks: A novel strategy to detect new targets in cancer therapy

Selga i Coma, Elisabet; Almagro García, Ma. Cristina de; Oleaga Sancho, Carlota; Mencía Trinchant, Núria; Ramírez, Sara; Ruiz, F. Xavier; Farrés i Vicén, Jaume; Parés i Casasampera, Xavier; Thibaut, Rémi; Porte Visa, Cinta; Noé Mata, Verónica; Ciudad i Gómez, Carlos Julián

Please use this identifier to cite or link to this item: https://hdl.handle.net/2445/21368

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DC Field	Value	Language
dc.contributor.author	Selga i Coma, Elisabet	cat
dc.contributor.author	Almagro García, Ma. Cristina de	cat
dc.contributor.author	Oleaga Sancho, Carlota	cat
dc.contributor.author	Mencía Trinchant, Núria	cat
dc.contributor.author	Ramírez, Sara	cat
dc.contributor.author	Ruiz, F. Xavier	cat
dc.contributor.author	Farrés i Vicén, Jaume	cat
dc.contributor.author	Parés i Casasampera, Xavier	cat
dc.contributor.author	Thibaut, Rémi	cat
dc.contributor.author	Porte Visa, Cinta	cat
dc.contributor.author	Noé Mata, Verónica	cat
dc.contributor.author	Ciudad i Gómez, Carlos Julián	cat
dc.date.accessioned	2012-01-09T09:18:20Z	-
dc.date.available	2012-01-09T09:18:20Z	-
dc.date.issued	2011	-
dc.identifier.uri	https://hdl.handle.net/2445/21368	-
dc.description	Podeu consultar el llibre complet a: http://www.trnres.com/ebookcontents.php?id=149	-
dc.description.abstract	The aim of this work was to design a novel strategy to detect new targets for anticancer treatments. The rationale was to build Biological Association Networks from differentially expressed genes in drug-resistant cells to identify important nodes within the Networks. These nodes may represent putative targets to attack in cancer therapy, as a way to destabilize the gene network developed by the resistant cells to escape from the drug pressure. As a model we used cells resistant to methotrexate (MTX), an inhibitor of DHFR. Selected node-genes were analyzed at the transcriptional level and from a genotypic point of view. In colon cancer cells, DHFR, the AKR1 family, PKC¿, S100A4, DKK1, and CAV1 were overexpressed while E-cadherin was lost. In breast cancer cells, the UGT1A family was overexpressed, whereas EEF1A1 was overexpressed in pancreatic cells. Interference RNAs directed against these targets sensitized cells towards MTX.	eng
dc.format.extent	33 p.	-
dc.format.mimetype	application/pdf	-
dc.language.iso	eng	eng
dc.publisher	Transworld Research Network	eng
dc.relation.isformatof	Reproducció del capítol 1 del llibre publicat a: http://www.trnres.com/ebookcontents.php?id=106	cat
dc.relation.ispartof	Recent Advances in Pharmaceutical Sciences, 2011, Chapter 1, p. 1-33. Editor: Diego Muñoz-Torrero	-
dc.relation.uri	http://hdl.handle.net/2445/32392	-
dc.rights	(c) Transworld Research Network, 2011	-
dc.source	Llibres / Capítols de llibre (Bioquímica i Biomedicina Molecular)	-
dc.subject.classification	Càncer	cat
dc.subject.classification	Quimioteràpia	cat
dc.subject.classification	Farmacogenètica	cat
dc.subject.other	Cancer	eng
dc.subject.other	Chemotherapy	eng
dc.subject.other	Pharmacogenetics	eng
dc.title	Generation of biological association networks: A novel strategy to detect new targets in cancer therapy	eng
dc.type	info:eu-repo/semantics/bookPart	-
dc.type	info:eu-repo/semantics/publishedVersion	-
dc.identifier.idgrec	249207	-
dc.date.updated	2011-12-27T14:10:22Z	-
dc.rights.accessRights	info:eu-repo/semantics/openAccess	-
Appears in Collections:	Llibres / Capítols de llibre (Bioquímica i Biomedicina Molecular)

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