Targeting MCT-1 oncogene inhibits Shc pathway and xenograft tumorigenicity

نویسندگان

  • Hung-Ju Shih
  • Hsiao-Huei Chen
  • Yen-An Chen
  • Meng-Hsun Wu
  • Gan-Guang Liou
  • Wei-Wen Chang
  • Linyi Chen
  • Lu-Hai Wang
  • Hsin-Ling Hsu
چکیده

Overexpression of Shc adaptor proteins is associated with mitogenesis, carcinogenesis and metastasis. Multiple copies in T-cell malignancy 1 (MCT-1) oncoprotein promotes cell proliferation, survival and tumorigenic effects. Our current data show that MCT-1 is a novel regulator of Shc-Ras-MEK-ERK signaling and MCT-1 is significantly co-activated with Shc gene in human carcinomas. The knockdown of MCT-1 enhances apoptotic cell death accompanied with the activation of caspases and cleavage of caspase substrates under environmental stress. The cancer cell proliferation, chemo-resistance and tumorigenic capacity are proved to be effectively suppressed by targeting MCT-1. Accordingly, an important linkage between MCT-1 oncogenicity and Shc pathway in tumor development has now been established. Promoting MCT-1 expression by gene hyperactivation may be recognized as a tumor marker and MCT-1 may serve as a molecular target of cancer therapy.

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عنوان ژورنال:

دوره 3  شماره 

صفحات  -

تاریخ انتشار 2012