Data di Pubblicazione:
2012
Abstract:
Purpose: Pheochromocytomas (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.
Design: We 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.
Results: Sixteen 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.
Conclusions: Germline 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. Clin Cancer Res; 18(10); 2828–37. ©2012 AACR.
Design: We 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.
Results: Sixteen 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.
Conclusions: Germline 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. Clin Cancer Res; 18(10); 2828–37. ©2012 AACR.
Tipologia CRIS:
1.1 Articolo in rivista
Keywords:
Pheochromocytoma; Genetics
Elenco autori:
Burnichon, N; Cascón, A; Schiavi, F; Morales, Np; Comino Méndez, I; Abermil, N; Inglada Pérez, L; de Cubas, Aa; Amar, L; Barontini, M; de Quirós, Sb; Bertherat, J; Bignon, Yj; Blok, Mj; Bobisse, S; Borrego, S; Castellano, Maurizio; Chanson, P; Chiara, Md; Corssmit, Ep; Giacchè, M; de Krijger, Rr; Ercolino, T; Girerd, X; Gómez García, Eb; Gómez Graña, A; Guilhem, I; Hes, Fj; Honrado, E; Korpershoek, E; Lenders, Jw; Letón, R; Mensenkamp, Ar; Merlo, A; Mori, Luigi; Murat, A; Pierre, P; Plouin, Pf; Prodanov, T; Quesada Charneco, M; Qin, N; Rapizzi, E; Raymond, V; Reisch, N; Roncador, G; Ruiz Ferrer, M; Schillo, F; Stegmann, Ap; Suarez, C; Taschin, E; Timmers, Hj; Tops, Cm; Urioste, M; Beuschlein, F; Pacak, K; Mannelli, M; Dahia, Pl; Opocher, G; Eisenhofer, G; Gimenez Roqueplo, Ap; Robledo, M.
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