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MAX mutations cause hereditary and sporadic pheochromocytoma and paraganglioma.

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dc.contributor.authorBurnichon, Nelly
dc.contributor.authorCascon Soriano, Alberto
dc.contributor.authorSchiavi, Francesca
dc.contributor.authorMorales, Nicole Paes
dc.contributor.authorComino-Méndez, Iñaki
dc.contributor.authorAbermil, Nasséra
dc.contributor.authorInglada-Pérez, Lucía
dc.contributor.authorde Cubas, Aguirre A
dc.contributor.authorAmar, Laurence
dc.contributor.authorBarontini, Marta
dc.contributor.authorde Quirós, Sandra Bernaldo
dc.contributor.authorBertherat, Jérôme
dc.contributor.authorBignon, Yves-Jean
dc.contributor.authorBlok, Marinus J
dc.contributor.authorBobisse, Sara
dc.contributor.authorBorrego, Salud
dc.contributor.authorCastellano, Maurizio
dc.contributor.authorChanson, Philippe
dc.contributor.authorChiara, María-Dolores
dc.contributor.authorCorssmit, Eleonora P M
dc.contributor.authorGiacchè, Mara
dc.contributor.authorde Krijger, Ronald R
dc.contributor.authorErcolino, Tonino
dc.contributor.authorGirerd, Xavier
dc.contributor.authorGómez-García, Encarna B
dc.contributor.authorGómez-Graña, Alvaro
dc.contributor.authorGuilhem, Isabelle
dc.contributor.authorHes, Frederik J
dc.contributor.authorHonrado, Emiliano
dc.contributor.authorKorpershoek, Esther
dc.contributor.authorLenders, Jacques W M
dc.contributor.authorLetón, Rocío
dc.contributor.authorMensenkamp, Arjen R
dc.contributor.authorMerlo, Anna
dc.contributor.authorMori, Luigi
dc.contributor.authorMurat, Arnaud
dc.contributor.authorPierre, Peggy
dc.contributor.authorPlouin, Pierre-François
dc.contributor.authorProdanov, Tamara
dc.contributor.authorQuesada-Charneco, Miguel
dc.contributor.authorQin, Nan
dc.contributor.authorRapizzi, Elena
dc.contributor.authorRaymond, Victoria
dc.contributor.authorReisch, Nicole
dc.contributor.authorRoncador, Giovanna
dc.contributor.authorRuiz-Ferrer, Macarena
dc.contributor.authorSchillo, Frank
dc.contributor.authorStegmann, Alexander P A
dc.contributor.authorSuarez, Carlos
dc.contributor.authorTaschin, Elisa
dc.contributor.authorTimmers, Henri J L M
dc.contributor.authorTops, Carli M J
dc.contributor.authorUrioste, Miguel
dc.contributor.authorBeuschlein, Felix
dc.contributor.authorPacak, Karel
dc.contributor.authorMannelli, Massimo
dc.contributor.authorDahia, Patricia L M
dc.contributor.authorOpocher, Giuseppe
dc.contributor.authorEisenhofer, Graeme
dc.contributor.authorGimenez-Roqueplo, Anne-Paule
dc.contributor.authorRobledo, Mercedes
dc.contributor.funderInstituto de Salud Carlos III
dc.contributor.funderfundacion MUTUA MADRILEÑA
dc.contributor.funderJUNTA DE ANDALUCIA
dc.contributor.funderAgence Nationale de la Recherche (ANR)
dc.contributor.funderUnited States Department of Health & Human Services National Institutes of Health (NIH) - USA
dc.date.accessioned2025-01-20T12:32:29Z
dc.date.available2025-01-20T12:32:29Z
dc.date.issued2012-05-15
dc.description.abstractPheochromocytomas (PCC) and paragangliomas (PGL) are genetically heterogeneous neural crest-derived neoplasms. Recently we identified germline mutations in a new tumor suppressor susceptibility gene, MAX (MYC-associated factor X), which predisposes carriers to PCC. How MAX mutations contribute to PCC/PGL and associated phenotypes remain unclear. This study aimed to examine the prevalence and associated phenotypic features of germline and somatic MAX mutations in PCC/PGL.
dc.description.abstractWe sequenced MAX in 1,694 patients with PCC or PGL (without mutations in other major susceptibility genes) from 17 independent referral centers. We screened for large deletions/duplications in 1,535 patients using a multiplex PCR-based method. Somatic mutations were searched for in tumors from an additional 245 patients. The frequency and type of MAX mutation was assessed overall and by clinical characteristics.
dc.description.abstractSixteen MAX pathogenic mutations were identified in 23 index patients. All had adrenal tumors, including 13 bilateral or multiple PCCs within the same gland (P < 0.001), 15.8% developed additional tumors at thoracoabdominal sites, and 37% had familial antecedents. Age at diagnosis was lower (P = 0.001) in MAX mutation carriers compared with nonmutated cases. Two patients (10.5%) developed metastatic disease. A mutation affecting MAX was found in five tumors, four of them confirmed as somatic (1.65%). MAX tumors were characterized by substantial increases in normetanephrine, associated with normal or minor increases in metanephrine.
dc.description.abstractGermline mutations in MAX are responsible for 1.12% of PCC/PGL in patients without evidence of other known mutations and should be considered in the genetic work-up of these patients.
dc.description.peerreviewedNo
dc.description.tableofcontentsThe ENS@T consortium received funding from the European Union Seventh Framework Programme (ENS@T-CANCER; HEALTH-F2-2010-259735). The ENS@T registry is supported by a grant of the European Science Foundation (ESF-ENS@T). This work was supported in part by the Fondo de Investigaciones Sanitarias (projects PI11/01359, PS09/00942, PI10/01290, PI08/0531 and P108/0883), Mutua Madrilena (AP2775/2008), Consejeria de Innovacion Ciencia y Empresa de la Junta de Andalucia (CTS-2590), Red Tematica de Investigacion Cooperativa en Cancer (RD06/0020/0034). The French COMETE network is supported in part by the Programme Hospitalier de Recherche Clinique grant COMETE 3(AOM 06 179), by grants from INSERM and Ministere Delegue a la Recherche et des Nouvelles Technologies and by the Institut National du Cancer. This work was also funded by grants from the Agence Nationale de la Recherche (ANR 08 GENOPATH 029 MitOxy) and by the national program "Cartes d'Identite des Tumeurs" funded and developed by the "Ligue Nationale contre le Cancer" (http://cit.ligue-cancer.net). This research was supported, in part, by the Intramural Research Program of the NIH, NICHD. This work received funding support from the Voelcker Fund to P. L. M. Dahia. This work was also supported in part by grants from the Fondazione Comunita Bresciana and the Fondazione Guido Berlucchi.
dc.format.number10
dc.format.page2828-2837
dc.format.volume18
dc.identifier.citationClin Cancer Res . 2012 May 15;18(10):2828-37
dc.identifier.journalCLINICAL CANCER RESEARCH
dc.identifier.pubmedID22452945
dc.identifier.urihttps://hdl.handle.net/20.500.12105/26068
dc.language.isoeng
dc.publisherAACR
dc.relation.projectIDinfo:eu-repo/grantAgreement/MICINN//PI11%2F01359/ES/Uso de plataformas de análisis masivo en el estudio de tumores endocrinos: de la OMICA al paciente: de la OMICA al paciente/
dc.relation.projectIDinfo:eu-repo/grantAgreement/MICINN//PS09%2F00942/ES/ULTRASECUENCIACION DE REGIONES RECURRENTES DE PERDIDA DE HETEROCIGOSIDAD EN PACIENTES CON FEOCROMOCITOMA FAMILIAR NO ASOCIADO A MUTACIONES EN LOS GENES DE SUSCEPTIBILIDAD CONOCIDOS/
dc.relation.projectIDP
dc.relation.publisherversionHTTP://doi: 10.1158/1078-0432.CCR-12-0160.
dc.repisalud.institucionCNIO
dc.repisalud.orgCNIOCNIO::Grupos de investigación::Grupo de Cáncer Endocrino Hereditario
dc.rights.accessRightsopen access
dc.rights.licenseAttribution-NonCommercial-NoDerivatives 4.0 International
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/4.0/
dc.titleMAX mutations cause hereditary and sporadic pheochromocytoma and paraganglioma.
dc.typeresearch article
dc.type.hasVersionAM
dspace.entity.typePublication
relation.isAuthorOfPublication610499dd-7ca3-4e9a-8b44-e5489f9212ab
relation.isAuthorOfPublication.latestForDiscovery610499dd-7ca3-4e9a-8b44-e5489f9212ab

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