Mechanisms underlying constitutive activation and oncogenic potential of mutant c-kit receptor tyrosine kinase

• Project/Area Number: 11670998
• Research Category: Grant-in-Aid for Scientific Research (C)
• Allocation Type: Single-year Grants
• Section: 一般
• Research Field: Hematology
• Research Institution: Osaka University
• Principal Investigator: IKEDA Hirokazu Osaka University Graduate School of Medicine, Assistant Professor, 医学系研究科, 助手 (10311755)
• Co-Investigator(Kenkyū-buntansha): KITAYAMA Hitoshi Osaka University Graduate School of Medicine, Assistant Professor, 医学系研究科, 助手 ; MATSUMURA Itaru Osaka University Graduate School of Medicine, Assistant Professor, 医学系研究科, 助手 (00294083) ; KANAKURA Yuzuru Osaka University Graduate School of Medicine, Professor, 医学系研究科, 教授 (20177489)
• Project Period (FY): 1999 – 2000
• Project Status: Completed (Fiscal Year 2000)
• Budget Amount: ¥3,500,000 (Direct Cost: ¥3,500,000); Fiscal Year 2000: ¥1,200,000 (Direct Cost: ¥1,200,000); Fiscal Year 1999: ¥2,300,000 (Direct Cost: ¥2,300,000)
• Keywords: c-kit receptor tyrosine kinase / oncogenic mutation / molecular target / tyrosine kinase inhibitor / tyrophostine / natural killer / T-cell lymphoma / naturalkiller / 二量体化 / ras

Research Abstract

The c-kit receptor tyrosine kinase(KIT)plays important roles in embryonhic development, *ematopoiesis and also malignant transformation. We revealed that two point mutations, Val559-->Gly(G559)mutation in the juxtamembrane domain and Asp814-->Val(V814)mutation in the kinase domain, lead to constitutive and oncogenic activation of KIT.Since oncogenic mutants seem to alter their conformation and substrate specificity compared with wild-type(WT)KIT, they may be preferentially inhibited by some compound. Tyrophostines are a class of tyrosine kinase inhibitor either through competition for substrate on through ATP binding. When KIT-WT, KIT-G559 and KIT-V814 expression vector were transfected into an embryonic kidney cell line 293T and treated with increasing dose of tyrophostin AG1296, kinase activity of KIT-G559 protein was more effectively inhibited than that of KIT-WT, whereas that of KIT-V814 was not affected at all. When these KIT genes were introduced into a murine interleukin(IL)-3-d ependent cell line Ba/F3, Ba/F3-KIT-WT showed Stem Cell Factor(SCF)-dependent, while Ba/F3-KIT-G559 and Ba/F3-KIT-V814 factor-independent. AG1296 inhibited both factor-independent growth of Ba/F3-KIT-G559 and SCF-dependent growth of Ba/F3-KIT-WT in a dose dependent manner but with different potencies. AG1296 had no effect on factor-independent growth of Ba/F3-KIT-V814 or IL-3-dependent growth of Ba/F3-mock. AG1296 inhibited activation of MAP kinase more effectively in Ba/F3-KIT-G559 than in Ba/F3-KIT-WT.Furthermore, AG1296 blocked antiapoptotic activity of KIT-G559 more potently than that of KIT-WT.These results suggest that a gain-of-function KIT mutant may be used as a molecular target for cancer therapy.
Sinonasal natural killer/T-cell lymphoma is one of the major constituents of lethal midline granuloma. Since natural killerT cell expresses c-kit, we examined c-kit mutation in these cases by PCR-SSCP followed by direct sequencing. Twelve single nucleotide substitution mutations were seen in 23 cases. Furthermore, seven of eight mutations(92%)in exon 17 occurred at codon 825 and three of four mutations(75%)in exon 11 occurred at codon 56l. Although the codon 825 mutation was not a gain-of-function mutation, the mechanisms of these mutations in pathogenesis are investigated.

Research Products

• [Publications] Hongyo T., et al.: "Specific c-kit mutations in sinonasal natural killer/T-cell lymphoma in China and Japan."Cancer Res.. 60. 2345-2347 (2000)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Daino, H., et al.: "Induction of apoptosis by extracellular ubiquitin in human hematopoietic cells : possible involve-ment of STAT3 degradation by proteasome pathway in interleukin 6-dependent hematopoietic cells."Blood. 95. 2577-2585 (2000)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Hongyo T., et al: "Specific c-kit mutations in sinonasal natural killer/T-cell lymphoma in China and Japan."Cancer Res.. 60. 2345-2347 (2000)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Daino, H., et al: "Induction of apoptosis by extracellular ubiquitin in human hematopoietic cells : possible involve-ment of STAT3 degradation by proteasome pathway in interleukin 6-dependent hematopoietic cells."Blood. 95. 2577-2585 (2000)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Hongyo T., et al.: "Specific c-kit mutations in sinonasal natural killer/t-cell lymphoma in China and Japan."Cancer Res.. 60(9). 2345-2347 (2000)
• [Publications] Daino,H., et al.: "Induction of apoptosis by extracellular ubiquitin in human hematopoietic cells : possible involve-ment of STAT3 degradation by proteasome pathway in interleukin 6-dependent hematopoietic cells."Blood. 95(8). 2577-2585 (2000)
• [Publications] Tsujimura T.et al.: "Activating mutation in the catalytic domain of c-kit elicits hematooietic transformation by receptor self-association not at the ligand-induced dimerization site"Blood. 93. 1319-1329 (1999)
• [Publications] Daino H.et al.: "Induction of apoptosis by extracellular ubiquitin in human hematopoietic cells: possible involvement of STAT3 degradation by proteasome pathway in interleukin 6-dependent hematopoietic cells"Blood. (in press).
• [Publications] Matsumura I.et al.: "Transcriptional regulation of cyclin D1 promoter by STAT5: its involvement in cytokine-dependent growth of hematopoietic cells"EMBO J.. 18. 1367-1377 (1999)
• [Publications] Oritani K.et al.: "Both Stat3-activation and Stat3-independent BCL2 downregulation are important for interleukin-6-induced apoptosis of 1A9-M cells"Blood. 93. 1346-1354 (1999)