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Functional analysis of receptor tyrosine kinase mutations in lung cancer identifies oncogenic extracellular domain mutations of ERBB2 |
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| Authors: | Heidi Greulich Bethany Kaplan Philipp Mertins Tzu-Hsiu Chen Kumiko E Tanaka Cai-Hong Yun Xiaohong Zhang Se-Hoon Lee Jeonghee Cho Lauren Ambrogio Rachel Liao Marcin Imielinski Shantanu Banerji Alice H Berger Michael S Lawrence Jinghui Zhang Nam H Pho Sarah R Walker Wendy Winckler Gad Getz David Frank William C Hahn Michael J Eck D R Mani Jacob D Jaffe Steven A Carr Kwok-Kin Wong Matthew Meyerson |
| Affiliation: | Department of Medical Oncology, Center for Cancer Genome Discovery, and Cancer Biology, Dana-Farber Cancer Institute, Boston, MA 02115. |
| Abstract: | We assessed somatic alleles of six receptor tyrosine kinase genes mutated in lung adenocarcinoma for oncogenic activity. Five of these genes failed to score in transformation assays; however, novel recurring extracellular domain mutations of the receptor tyrosine kinase gene ERBB2 were potently oncogenic. These ERBB2 extracellular domain mutants were activated by two distinct mechanisms, characterized by elevated C-terminal tail phosphorylation or by covalent dimerization mediated by intermolecular disulfide bond formation. These distinct mechanisms of receptor activation converged upon tyrosine phosphorylation of cellular proteins, impacting cell motility. Survival of Ba/F3 cells transformed to IL-3 independence by the ERBB2 extracellular domain mutants was abrogated by treatment with small-molecule inhibitors of ERBB2, raising the possibility that patients harboring such mutations could benefit from ERBB2-directed therapy. |
| Keywords: | HER2 breast cancer bladder cancer |
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