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The impact of human EGFR kinase domain mutations on lung tumorigenesis and in vivo sensitivity to EGFR-targeted therapies
Authors:Ji Hongbin  Li Danan  Chen Liang  Shimamura Takeshi  Kobayashi Susumu  McNamara Kate  Mahmood Umar  Mitchell Albert  Sun Yangping  Al-Hashem Ruqayyah  Chirieac Lucian R  Padera Robert  Bronson Roderick T  Kim William  Jänne Pasi A  Shapiro Geoffrey I  Tenen Daniel  Johnson Bruce E  Weissleder Ralph  Sharpless Norman E  Wong Kwok-Kin
Affiliation:Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts 02115, USA.
Abstract:To understand the role of human epidermal growth factor receptor (hEGFR) kinase domain mutations in lung tumorigenesis and response to EGFR-targeted therapies, we generated bitransgenic mice with inducible expression in type II pneumocytes of two common hEGFR mutants seen in human lung cancer. Both bitransgenic lines developed lung adenocarcinoma after sustained hEGFR mutant expression, confirming their oncogenic potential. Maintenance of these lung tumors was dependent on continued expression of the EGFR mutants. Treatment with small molecule inhibitors (erlotinib or HKI-272) as well as prolonged treatment with a humanized anti-hEGFR antibody (cetuximab) led to dramatic tumor regression. These data suggest that persistent EGFR signaling is required for tumor maintenance in human lung adenocarcinomas expressing EGFR mutants.
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