Prognosis and predictive value of KIT exon 11 deletion in GISTs

J. B. Bachet, I. Hostein, A. Le Cesne, S. Brahimi, A. Beauchet, S. Tabone-Eglinger, F. Subra, B. Bui, F. Duffaud, P. Terrier, J. M. Coindre, J. Y. Blay, J. F. Emile

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    Résumé

    Background:KIT exon 11 mutations are observed in 60% of gastrointestinal stromal tumours (GIST). Exon 11 codes for residues Tyr568 and Tyr570, which play a major role in signal transduction and degradation of KIT. Our aim was to compare the outcome of patients with deletion of both Tyr568-570 (delTyr) and the most frequent deletion delWK557-558 (delWK).Methods:Pathology and clinical characteristics of 68 patients with delTyr (n26) or delWK (n42) were reviewed and compared.Results:GISTs with delTyr were more frequently extragastric than those with delWK (69 vs 26%, P0.0005). After curative surgery, median relapse-free survival were 10.8 and 11.1 months for patients with delTyr (n14) and delWK (n29), respectively (P0.92). All patients treated with imatinib for a non-resectable or metastatic GIST had an objective response (n15) or a stable disease (n21) as best response, regardless of mutation. Median progression-free survival with imatinib were 21.9 and 18.9 months for patients with GIST with delTyr (n14) and delWK (n22), respectively (P0.43).Conclusion:In this large retrospective series, the type of KIT exon 11 mutation was correlated with the origin of GIST, but not with prognosis or response to imatinib.

    langue originaleAnglais
    Pages (de - à)7-11
    Nombre de pages5
    journalBritish Journal of Cancer
    Volume101
    Numéro de publication1
    Les DOIs
    étatPublié - 7 juil. 2009

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