MUTATION AND CLINICAL SIGNIFICANCE OF C-FMS ONCOGENE IN HEPATOCELLULAR CARCINOMA  被引量：1

作　　者：崔俊 杨冬华 毕向军 

出　　处：《Chinese Journal of Cancer Research》2001年第1期31-34,共4页中国癌症研究（英文版）

摘　　要：Objective: To study the clinical significance and relationship between c-fms oncogene and hepatocellular carcinogenesis, to further clarify the occurring mechanism of hepatocellular carcinoma (HCC). Methods: PCR-SSCP technique was used to analyse mutation of c-fms oncogene in 30 cases of HCC tissues. Sequencing the PCR products after cloning to prove the mutations, meanwhile the relationship between c-fms mutations and clinical pathology of HCC was investigated. Results: Two abnormal single strands were observed in 10% (3/30) HCC tissues from c-fms DNA corresponding to 301st codon of c-fms amino acids. PCR products of abnormal single strands were sequenced after cloning, it demonstrated that there was transition of T→C at nucleic acid 14855 of c-fms DNA, which corresponded to transition of Leu (TTG)→Ser (TCG) at 301st codon of c-fms amino acids. The mutation was related to malignant degree and type of HCC tissues as well as patient’s age. Conclusion: Mutation of c-fms codon at site 301 implied a molecular mechanism contributing to hepatocellular carcinogenesis.Objective: To study the clinical significance and relationship between c-fms oncogene and hepatocellular carcinogenesis, to further clarify the occurring mechanism of hepatocellular carcinoma (HCC). Methods: PCR-SSCP technique was used to analyse mutation of c-fms oncogene in 30 cases of HCC tissues. Sequencing the PCR products after cloning to prove the mutations, meanwhile the relationship between c-fms mutations and clinical pathology of HCC was investigated. Results: Two abnormal single strands were observed in 10% (3/30) HCC tissues from c-fms DNA corresponding to 301st codon of c-fms amino acids. PCR products of abnormal single strands were sequenced after cloning, it demonstrated that there was transition of T→C at nucleic acid 14855 of c-fms DNA, which corresponded to transition of Leu (TTG)→Ser (TCG) at 301st codon of c-fms amino acids. The mutation was related to malignant degree and type of HCC tissues as well as patient’s age. Conclusion: Mutation of c-fms codon at site 301 implied a molecular mechanism contributing to hepatocellular carcinogenesis.

关 键 词：Hepatocellular carcinoma c-fms oncogene MUTATION 

分 类 号：R730.2[医药卫生—肿瘤]