<i>PDGFRA</i> Activating Mutations in Gastrointestinal Stromal Tumors

Michael C. Heinrich; Christopher L. Corless; Anette Duensing; Laura McGreevey; Chang-Jie Chen; Nora Joseph; Samuel Singer; Diana Griffith; Andrea Haley; Ajia Town; George D. Demetri; Christopher D.�M. Fletcher; Jonathan A. Fletcher

doi:10.1126/science.1079666

<i>PDGFRA</i> Activating Mutations in Gastrointestinal Stromal Tumors

Michael C. Heinrich(Oregon Health & Science University), Christopher L. Corless(Portland VA Medical Center), Anette Duensing(Brigham and Women's Hospital), Laura McGreevey(Oregon Health & Science University), Chang-Jie Chen(Brigham and Women's Hospital), Nora Joseph(Brigham and Women's Hospital), Samuel Singer(Memorial Sloan Kettering Cancer Center), Diana Griffith(Oregon Health & Science University), Andrea Haley(Oregon Health & Science University), Ajia Town(Oregon Health & Science University), George D. Demetri(Harvard University), Christopher D.�M. Fletcher(Brigham and Women's Hospital), Jonathan A. Fletcher(Brigham and Women's Hospital)

Science

January 30, 2003

10.1126/science.1079666

Cited by 2,288

Abstract

Most gastrointestinal stromal tumors (GISTs) have activating mutations in the KIT receptor tyrosine kinase, and most patients with GISTs respond well to Gleevec, which inhibits KIT kinase activity. Here we show that approximately 35% (14 of 40) of GISTs lacking KIT mutations have intragenic activation mutations in the related receptor tyrosine kinase, platelet-derived growth factor receptor alpha (PDGFRA). Tumors expressing KIT or PDGFRA oncoproteins were indistinguishable with respect to activation of downstream signaling intermediates and cytogenetic changes associated with tumor progression. Thus, KIT and PDGFRA mutations appear to be alternative and mutually exclusive oncogenic mechanisms in GISTs.

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