High expression of both mutant and wild-type alleles of c-kit in gastrointestinal stromal tumors

Nathalie Théou, Séverine Tabone, Raphael Saffroy, Axel Le Cesne, Catherine Julié, Annie Cortez, Anne Lavergne-Slove, Brigitte Debuire, Antoinette Lemoine, Jean François Emile

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    Résumé

    Most gastrointestinal stromal tumors (GISTs) contain activating mutations of the proto-oncogene c-kit. The GNNK- isoform of c-kit has a greater oncogenic potential than the GNNK+ isoform. We studied tumors from 29 patients with GIST, 19 of whom had c-kit mutations, and compared them to normal cells and HMC-1 mast cell line. c-kit transcripts were quantified by real-time PCR. The ratios of GNNK-/+ isoforms and of wild-type/mutant alleles were determined by RT-PCR and fluorometric quantification. On average, GISTs contained 1.9 times more c-kit transcripts than the HMC-1 cell line and GISTs with c-kit mutations contained 2.8 times more c-kit transcripts than those without (P=0.003). The median GNNK-/+ isoform ratios in GISTs with and without c-kit mutations were 4. 4 and 4.1, respectively, and there was no difference in the GNNK-/+ ratios between the GISTs and the control samples. Both mutant and wild-type alleles of c-kit were expressed in similar amounts in 13/15 mutant GISTs. The oncogenic effects of KIT in GISTs are not related to the higher expression level of the GNNK- isoform. The high expression level of both mutated and wild-type allele transcripts of c-kit suggests that interactions between spontaneously activated and normal c-kit receptors are important in GIST tumorigenesis.

    langue originaleAnglais
    Pages (de - à)250-256
    Nombre de pages7
    journalBiochimica et Biophysica Acta - Molecular Basis of Disease
    Volume1688
    Numéro de publication3
    Les DOIs
    étatPublié - 5 avr. 2004

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