汤绍辉,杨冬华,罗和生,于皆平,舒建昌.CDKN2A位点p16INK4α、p14ARF基因变异与胃癌发生的关系[J].Chinese journal of Epidemiology,2004,25(6):517-520,521 |
CDKN2A位点p16INK4α、p14ARF基因变异与胃癌发生的关系 |
Relationship between alterations of p16INK4a and p14ARF genes of CDKN2A locus and gastric carcinogenesis |
Received:April 08, 2003 |
DOI: |
KeyWord: 胃肿瘤 基因 |
English Key Word: Gastric cancer Genes |
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Abstract: |
目的 探讨p16INK4a和p14ARF基因变异与胃癌发生的关系。方法 应用聚合酶链反应(PCR)、PCR-单链构象多态性(SSCP)、PCR甲基化分析法和RT-PCR分别检测48例胃癌及癌旁组织中p16INK4a和p14ARF基因纯合性缺失、突变、CpG岛甲基化及mRNA表达状况。结果(1)胃癌组织p16INK4a和p14ARF基因总缺失率为35.4%(17/48),癌旁组织均未见纯合性缺失。(2)31例无纯合性缺失的胃癌及癌旁组织均未见p16INK4a和p14ARF基因点突变。(3)胃癌组织p16INK4a和p14ARF基因总甲基化率为47.90%(23/48),癌旁组织仅2例甲基化,两者差异有显著性(P<0.01)。(4)胃癌组织p16INK4amRNA缺失率为47.9%(23/48),其中E1α和E2共甲基化者p16INK4amRNA缺失率(100%,6/6)明显高于其他类型甲基化者(11.8%,2/17)(P<0.01);胃癌组织p14ARFmRNA缺失率为45.8%(22/48),其中E1β和E2共甲基化者p14ARFmRNA缺失率(100%,3/3)明显高于其他类型甲基化者(15%,3/20)(P<0.05)。(5)低未分化癌组p16INK4a和p14ARFmRNA共同缺失率(36.7%,11/30)明显高于高中分化癌组(5.6%,1/18)(P<;0.05)。结论 胃癌中p16INK4a和p14ARF基因失活多由纯合性缺失和5’CpG岛甲基化所致,其表达缺失与胃癌的发生密切相关。 |
English Abstract: |
Objective To investigate the relationship between alterations of p16INK4a and P14ARF genes and gastric carcinogenesis.Methods Tumors and gastric tissues neighboring carinoma from 48 patients with gastric cancer were studied. Homozygous deletion,mutation,methylation of the CpG islands,mRNA expression of p16INK4a and p14ARF genes were assessed by polymerase chain reaction(PCR),PCR-single strand conformation polymorphism(SSCP),PCR based methylation assay,and reverse transcription (RT)-PCR.Results (1)The overall homozygous deletion rate of p16INK4a,and p14AR was 35.4% (17/ 48),and no homozygous deletion was examined in all the gastric tissues neighboring tumor.(2)There was no pont mutation of p16INK4a and p14ARF in 31 gastric cancers without homozygous deletion and in the matched gastric tissues adjacent to tumor.(3)Methylation of the CpG islands of p16INK4a and p14ADF was detected in 47.9% (23/48) of gastric cancers,while methylation was observed only in 2 of 48 gastric tissues neighboring cancers with a significant difference (P0.01).(4) The rate of p16INK4a mRNA loss was 47.9% (23/48) in gastric cancer,and the cases of comined methylation of exons 1α and 2 had a higher be rate (100%, 6/6) of p16INK4a mRNA than those of methylation form the other exons(11.8%,2/17) (P0.01).The be rate of p14ARF mRNA was 45.8%(22/48) in gastric cancer,and patients with combined methylation of exons 1β and 2 had a higher loss rate (100%,3/3) of p14ARF mRNA than those of the methylation from the other exons (15%,3/20) (P0.05).(5)The combined loss of p16INK4a and p14ARF mRNAs was examined in 1(5.6%) of 18 cases of well and moderately-differentiated carcinomas,and 11 (36.7%) of 30 cases of poorly and not-differentiated carcinomas with significan difference(P0.05).Conclusion p16INK4a and p14ARF genes were frequently inactivated by homozygous deletion and methylation of the 5' CpG islands in gastric cancer,which might have played an important role in the development of gastric cancer. |
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