摘要
AIM:To investigate the mutational features of adenomatous polyposis coil (APC) gene and its possible arising mechanism in hereditary non-polyposis colorectal cancers (HNPCC).METHODS: PCR-based In Vitro Synthesized Protein Test (IVSP) assay and sequencing analysis were used to confirm somatic mutations of whole APC gene in 19 HNPCC cases.RESULTS: Eleven cases with 13 mutations were determined to harbor APC mutations. The prevalence of APC mutation was 58%(11/19). The mutations consisted of 9 frameshift and 4 nonsense ones, indicating that there were more frameshift mutations (69%).The frameshift mutations all exhibited deletion or insertion of 1-2 bp and most of them (7/9) happened at simple nucleotide repeat sequences,particularly within (A)n tracts (5/9). All point mutations presented C-to-T transitions at CpG sites.CONCLUSION: Mutations of APC gene were detected in more than half of HNPCC, indicating that its mutation was a common molecular event and might play an important role in the tumorigenesis of HNPCC. Locations of frameshift mutations at simple nucleotide repeat sequences and point mutations at CpG sites suggested that many mutations probably derived from endogenous processes including mismatch repair (MMR) deficiency. Defective MMR might affect the nature of APC mutations in HNPCC and likely occur earlier than APC mutational inactivation in some patients.
AIM:To investigate the mutational features of adenomatous polyposis coli (APC) gene and its possible arising mechanism in hereditary non-polyposis colorectal cancers (HNPCC). METHODS:PCR-based In Vitro Synthesized Protein Test (IVSP) assay and sequencing analysis were used to confirm somatic mutations of whole APC gene in 19 HNPCC cases. RESULTS:Eleven cases with 13 mutations were determined to harbor APC mutations.The prevalence of APC mutation was 58%(11/19).The mutations consisted of 9 frameshift and 4 nonsense ones,indicating that there were more frameshift mutations (69%).The frameshift mutations all exhibited deletion or insertion of 1-2 bp and most of them (7/9) happened at simple nucleotide repeat sequences, particularly within (A)n tracts (5/9).All point mutations presented C-to-T transitions at CpG sites. CONCLUSION:Mutations of APC gene were detected in more than half of HNPCC,indicating that its mutation was a common molecular event and might play an important role in the tumorigenesis of HNPCC.Locations of frameshift mutations at simple nucleotide repeat sequences and point mutations at CpG sites suggested that many mutations probably derived from endogenous processes including mismatch repair (MMR) deficiency.Defective MMR might affect the nature of APC mutations in HNPCC and likely occur earlier than APC mutational inactivation in some patients.
基金
Supported by the National Natural Science Foundation of China,No.39600055
Research for Returned Chinese Visiting Scholars from Abroad,Chinese Ministry of Education and Research of Provincial Education Ministry
