Oncogenic MAP2K1 mutations in human epithelial tumors

被引:40
作者
Choi, Young Lim [1 ,2 ]
Soda, Manabu [1 ]
Ueno, Toshihide [1 ]
Hamada, Toru [1 ]
Haruta, Hidenori [1 ]
Yamato, Azusa [1 ]
Fukumura, Kazutaka [2 ]
Ando, Mizuo [2 ]
Kawazu, Masahito [2 ]
Yamashita, Yoshihiro [1 ]
Mano, Hiroyuki [1 ,2 ,3 ]
机构
[1] Jichi Med Univ, Div Funct Genom, Shimotsuke, Tochigi 3290498, Japan
[2] Univ Tokyo, Grad Sch Med, Dept Med Genom, Tokyo 1130033, Japan
[3] Japan Sci & Technol Agcy, Kawaguchi, Saitama 3320012, Japan
基金
日本学术振兴会;
关键词
CELL LUNG-CANCER; KINASE; MEK1; GENE; BRAF; RAS; IDENTIFICATION; INHIBITION; THERAPY;
D O I
10.1093/carcin/bgs099
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The scirrhous subtype of gastric cancer is a highly infiltrative tumor with a poor outcome. To identify a transforming gene in this intractable disorder, we constructed a retroviral complementary DNA (cDNA) expression library from a cell line (OCUM-1) of scirrhous gastric cancer. A focus formation assay with the library and mouse 3T3 fibroblasts led to the discovery of a transforming cDNA, encoding for MAP2K1 with a glutamine-to-proline substitution at amino acid position 56. Interestingly, treatment with a MAP2K1-specific inhibitor clearly induced cell death of OCUM-1 but not of other two cells lines of scirrhous gastric cancer that do not carry MAP2K1 mutations, revealing the essential role of MAP2K1(Q56P) in the transformation mechanism of OCUM-1 cells. By using a next-generation sequencer, we further conducted deep sequencing of the MAP2K1 cDNA among 171 human cancer specimens or cell lines, resulting in the identification of one known (D67N) and four novel (R47Q, R49L, I204T and P306H) mutations within MAP2K1. The latter four changes were further shown to confer transforming potential to MAP2K1. In our experiments, a total of six (3.5%) activating mutations in MAP2K1 were thus identified among 172 of specimens or cell lines for human epithelial tumors. Given the addiction of cancer cells to the elevated MAP2K1 activity for proliferation, human cancers with such MAP2K1 mutations are suitable targets for the treatment with MAP2K1 inhibitors.
引用
收藏
页码:956 / 961
页数:6
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