摘要
目的为探讨非小细胞肺癌(NSCLC)细胞中第三号染色体短臂上3p25位点上等位基因的杂合性丢失(LossofHeterozygosityLOH)与肺癌发生发展的相关性。方法采用银染聚合酶链反应(PCR)结合二核苷酸(CA)n重复程序出现多态性评价杂合性丢失方法,分析58例NSCLC组织中3p25等位基因的杂合性丢失。结果58例肺癌组织中有29例出现3p25LOH,总的杂合性丢失率为50%。3p25的杂合性丢失率在18例腺癌中为12例(66.7%),明显高于鳞癌(42.9%,15/35),有显著性统计学意义(P<0.05),但3p25杂合性丢失与NSCLC临床分期关系不明显,Ⅰ期为42.1%,Ⅱ期为55.6%和Ⅲ期为52.2%,5例正常胎儿肺组织均不出现3p25LOH。结论3p25杂合性丢失在NSCLC中普遍存在,从而说明3p25位点处存在着某些与肺癌发生发展有关的抑癌基因。
bjective:Relationship between deletion of a wild type allele on chromosome 3p 14-25 and non small cell lung cancer(NSCLC)was studied.Methods:The 3p 25 loss of heterozygosity(LOH)was analysed in patients with NSCLC by polymerase chain reaction based assay for dinucleatied repeat polymorphisms.Results:Twenty nine(50%)out of 58 cases of NSCLC were found to have the LOH,but none in 5 embryonic lung tissues.This LOH frequency was 66 7% in adeno carcinoma and 42 9% in squamous cell carcinoma with significant difference between them ( P <0 05).The LOH frequency was not correlated with clinical TNM stages of NSCLC( P >0 05).Conclusions:Deletion of the wild type allele 3p 25 appeared to be a common structural alteration occurred in various types of lung cancer,and was an early molecular event involved in lung carcinogenesis.
出处
《肿瘤》
CAS
CSCD
北大核心
1997年第6期439-441,共3页
Tumor
基金
上海市科委课题
关键词
非小细胞
染色体畸变
3p^25
杂合性丢失
肺肿瘤
Non small cell lung cancer Chromosome 3p 25 Allele Loss of heterozygosity (LOH) PCR LOH analysis
