Mechanisms of oncogenic KIT signal transduction in primary gastrointestinal stromal tumors (GISTs)

生物 癌症研究 蛋白激酶B 信号转导 受体酪氨酸激酶 原癌基因蛋白质c-kit MAPK/ERK通路 甲磺酸伊马替尼 酪氨酸激酶 磷酸化 外显子 主旨 伊马替尼 间质细胞 细胞生物学 遗传学 干细胞因子 干细胞 髓系白血病 造血 基因
作者
Anette Duensing,Fabíola Medeiros,Bryna McConarty,Nora Joseph,Dipak Panigrahy,Samuel Singer,Christopher D.�M. Fletcher,George D. Demetri,Jonathan A. Fletcher
出处
期刊:Oncogene [Springer Nature]
卷期号:23 (22): 3999-4006 被引量:302
标识
DOI:10.1038/sj.onc.1207525
摘要

Most gastrointestinal stromal tumors (GISTs) express constitutively activated forms of the KIT receptor tyrosine kinase protein, resulting from oncogenic mutations in the extracellular, juxtamembrane, or kinase domains. KIT oncoproteins are detected early in GIST tumorigenesis, and most GIST patients respond well to treatment with the KIT kinase inhibitor imatinib mesylate (STI571, Gleevec®). However, GISTs can develop resistance to imatinib, and additional therapeutic strategies are needed. Little is known about oncogenic KIT signal transduction in GISTs, and whether the type of KIT mutation accounts for selective activation of downstream signaling intermediates. We therefore evaluated KIT downstream signaling profiles in 15 primary GISTs with mutations in KIT exons 9, 11, 13, and 17, and in two human GIST cell lines. All GISTs showed constitutive phosphorylation at KIT tyrosine residues Y703 and Y721. Additionally, most GISTs showed activation of MAPK p42/44, AKT, S6K, STAT1, and STAT3. STAT5 and JNK were not demonstrably activated in any GIST. Using GIST in vitro models, we showed that activation of MAPK p42/44, AKT, and S6K was KIT dependent, whereas STAT1 and STAT3 phosphorylation was only partially dependent on KIT activation. Correlation of activated signaling pathways with the type of KIT mutation revealed low levels of AKT phosphorylation in exon 9 mutant GISTs in contrast to a subset of GISTs with exon 11 mutations. However, additional factors are likely to modify the engagement of signaling pathways in GISTs as suggested by the fact that four GISTs with identical KIT exon 9 mutations had differential activation of MAPK p42/44 and STAT proteins. In summary, in this first report on KIT signal transduction in primary GISTs and GIST cell lines, we identified pathways that are constitutively activated in a KIT-dependent manner and therefore warrant further study as molecular targets in GISTs.

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