Higher risk of death among men1 patients with mutations in the jund interacting domain: A groupe d'étude des tumeurs endocrines (GTE) cohort study

Julien Thevenon, Abderrahmane Bourredjem, Laurence Faivre, Catherine Cardot-bauters, Alain Calender, Arnaud Murat, Sophie Giraud, Patricia Niccoli, Marie Françoise Odou, Françoise Borson-chazot, Anne Barlier, Catherine Lombard-bohas, Eric Clauser, Antoine Tabarin, Béatrice Parfait, Olivier Chabre, Emilie Castermans, Albert Beckers, Philippe Ruszniewski, Morgane Le brasBrigitte Delemer, Philippe Bouchard, Isabelle Guilhem, Vincent Rohmer, Bernard Goichot, Philippe Caron, Eric Baudin, Philippe Chanson, Lionel Groussin, Hélène Du boullay, Georges Weryha, Pierre Lecomte, Alfred Penfornis, Hélène Bihan, Françoise Archambeaud, Véronique Kerlan, Françoise Duron, Jean Marc Kuhn, Bruno Vergàs, Michel Rodier, Michel Renard, Jean Louis Sadoul, Christine Binquet, Pierre Goudet

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    Abstract

    Multiple endocrine neoplasia syndrome type 1 (MEN1), which is secondary to mutation of the MEN1 gene, is a rare autosomal-dominant disease that predisposes mutation carriers to endocrine tumors. Although genotype-phenotype studies have so far failed to identify any statistical correlations, some families harbor recurrent tumor patterns. The function of MENIN is unclear, but has been described through the discovery of its interacting partners. Mutations in the interacting domains of MENIN functional partners have been shown to directly alter its regulation abilities. We report on a cohort of MEN1 patients from the Groupe d'étude des Tumeurs Endocrines. Patients with a molecular diagnosis and a clinical follow-up, totaling 262 families and 806 patients, were included. Associations between mutation type, location or interacting factors of the MENIN protein and death as well as the occurrence of MEN1-related tumors were tested using a frailty Cox model to adjust for potential heterogeneity across families. Accounting for the heterogeneity across families, the overall risk of death was significantly higher when mutations affected the JunD interacting domain (adjusted HR = 1.88: 95%-CI = 1.15-3.07). Patients had a higher risk of death from cancers of the MEN1 spectrum (HR = 2.34; 95%-CI = 1.23-4.43). This genotype-phenotype correlation study confirmed the lack of direct genotype-phenotype correlations. However, patients with mutations affecting the JunD interacting domain had a higher risk of death secondary to a MEN1 tumor and should thus be considered for surgical indications, genetic counseling and follow-up.

    Original languageEnglish
    Article numberddt039
    Pages (from-to)1940-1948
    Number of pages9
    JournalHuman Molecular Genetics
    Volume22
    Issue number10
    DOIs
    Publication statusPublished - 1 May 2013

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