Frontiers in Molecular Biosciences (Jun 2022)

Rare c-KIT c.1926delA and c.1936T>G Mutations in Exon 13 Define Imatinib Resistance in Gastrointestinal Stromal Tumors and Melanoma Patients: Case Reports and Cell Experiments

  • Chi Yan,
  • Chi Yan,
  • Chengzhi Zhao,
  • Chengzhi Zhao,
  • Ke Yang,
  • Ke Yang,
  • Hongyan Zhou,
  • Limin Jing,
  • Weixing Zhao,
  • Wenguang Dou,
  • Qingxin Xia,
  • Jie Ma,
  • Jie Ma,
  • Bing Wei,
  • Bing Wei,
  • Yongjun Guo,
  • Yongjun Guo

DOI
https://doi.org/10.3389/fmolb.2022.730213
Journal volume & issue
Vol. 9

Abstract

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Background: Target therapies play more and more important roles in gastrointestinal stromal tumors (GISTs) and melanoma with the advancement of clinical drugs that overcome the resistance caused by gene mutations. c-KIT gene mutations account for a large portion of GIST patients, which are known to be sensitive or resistant to tyrosine kinase inhibitors. However, the role rare mutations play in drug efficacy and progression-free duration remains elusive.Methods: Two rare mutations were identified using Sanger sequencing from the GIST and melanoma cases. Cell experiments were further carried out to demonstrate their role in the imatinib resistance.Results:c-KIT c.1926delA p.K642S*FS mutation in primary and recurrent GIST patients and c-KIT c.1936T>G p.Y646D point mutation in melanoma patients in exon 13 were first demonstrated to be novel targets resistant to imatinib agent.Conclusion:c-KIT mutations c.1926delA and c.1936T>G in exon 13 are clinically significant targets that exhibit resistance to imatinib. This study provides guidance to GIST and melanoma treatments.

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