Novel mutations of the MET proto-oncogene in papillary renal carcinomas.

6533b854fe1ef96bd12adf24

RESEARCH PRODUCT

Novel mutations of the MET proto-oncogene in papillary renal carcinomas.

Noboru Nakaigawa M. Miller J. A. Brown Kerstin Junker W. M. Linehan Robert B. Jenkins Hartmut P. H. Neumann Stéphane Richard Ulf S.r. Bergerheim T. Kinjerski Laura S. Schmidt Michael Dean Irina A. Lubensky Bernard Gerrard Cathy D. Vocke Jochen Decker Berton Zbar Gregor Weirich Hiltrud Brauch

subject

Adenoma Models Molecular Cancer Research Protein Conformation DNA Mutational Analysis Molecular Sequence Data Hereditary Papillary Renal Cell Carcinoma Biology medicine.disease_cause Transfection Proto-Oncogene Mas Receptor tyrosine kinase Mice Adenosine Triphosphate Neoplastic Syndromes Hereditary Proto-Oncogenes Genetics Carcinoma medicine Missense mutation Animals Humans Point Mutation Amino Acid Sequence Phosphorylation Codon Molecular Biology Kidney Mutation Binding Sites Sequence Homology Amino Acid Point mutation 3T3 Cells DNA Neoplasm Proto-Oncogene Proteins c-met medicine.disease Carcinoma Papillary Kidney Neoplasms Neoplasm Proteins medicine.anatomical_structure Cell Transformation Neoplastic Cancer research biology.protein Mutagenesis Site-Directed Tyrosine kinase Protein Processing Post-Translational Sequence Alignment

description

Hereditary papillary renal carcinoma (HPRC) is characterized by multiple, bilateral papillary renal carcinomas. Previously, we demonstrated missense mutations in the tyrosine kinase domain of the MET proto-oncogene in HPRC and a subset of sporadic papillary renal carcinomas. In this study, we screened a large panel of sporadic papillary renal carcinomas and various solid tumors for mutations in the MET proto-oncogene. Summarizing these and previous results, mutations of the MET proto-oncogene were detected in 17/129 sporadic papillary renal carcinomas but not in other solid tumors. We detected five novel missense mutations; three of five mutations were located in the ATP-binding region of the tyrosine kinase domain of MET. One novel mutation in MET, V1110I, was located at a codon homologous to an activating mutation in the c-erbB proto-oncogene. These mutations caused constitutive phosphorylation of MET when transfected into NIH3T3 cells. Molecular modeling studies suggest that these activating mutations interfere with the intrasteric mechanism of tyrosine kinase autoinhibition and facilitate transition to the active form of the MET kinase. The low frequency of MET mutations in noninherited papillary renal carcinomas (PRC) suggests that noninherited PRC may develop by a different mechanism than hereditary papillary renal carcinoma.

year	journal	country	edition	language
1999-05-18	Oncogene

10.1038/sj.onc.1202547 https://pubmed.ncbi.nlm.nih.gov/10327054