食管与贲门双源癌蛋白质指纹模型的建立及肿瘤标志的筛选  被引量：12

作　　者：冯笑山[1] 王立东[1] 郭涛[1] 单探幽[2] 李吉林 范宗民[1] 焦新英 常智慧 韩晶[2] 宋昕[1] 高社干[1] 申秋[1] 樊慧[1] 王能超[1] 李韶华[1] 高珊珊[1] 何欣[1] 郭军辉[1] 

机构地区：[1]河南省食管癌重点开放实验室郑州大学基础医学院,河南郑州450052 [2]河南科技大学第一附属医院肿瘤科河南科技大学肿瘤研究所,河南洛阳471003 [3]林州市姚村食管癌医院病理科,河南林州456592 [4]林州市中心医院病理科,河南林州456550

出　　处：《中华肿瘤防治杂志》2007年第8期564-568,共5页Chinese Journal of Cancer Prevention and Treatment

基　　金：国家自然科学基金(30025016);国家科技部863重大项目(2007);河南省医学创新人才工程项目(200084)

摘　　要：目的:建立食管与贲门双源癌的蛋白质组指纹诊断模型,筛选食管贲门双源癌相关蛋白,为建立食管贲门双源癌肿瘤标志提供理论基础。方法:采用表面增强激光解吸离子化飞行时间质谱仪(SELDI-TOF-MS)技术对19例食管贲门双源癌(双源癌组)和50位健康人(对照组)的血清进行蛋白质组的对比研究。根据差异性蛋白质的质核比(相对分子质量)从SWISS-PROT蛋白质数据库中筛选并确定相关候选蛋白和基因。并通过RT-PCR方法进一步分析这些关键候选基因在食管贲门双源癌组织中表达变化特征。结果:以相对分子质量2.86621×103、5.10330×103、6.59765×103、7.93155×103、9.31196×103和4.11399×103的6种蛋白质组成的决策树模型对双源癌组诊断的准确率、敏感度和特异度分别为78.26%、73.68%和80%。相对分子质量为5.34052×103和5.92132×103的蛋白质查询结果为COX7c及Beta-defensin-1-2-3,在双源癌的食管癌组织和贲门癌组织的阳性率分别为60%(3/5)、60%(3/5)、60%(3/5)和40%(2/5),对照组食管和贲门正常上皮组织均为阴性。结论:以相对分子质量2.86621×103、5.10330×103、6.59765×103、7.93155×103、9.31196×103和4.11399×103的6种蛋白质组成的决策树模型,可作为食管贲门双源癌的蛋白诊断模型,COX7c及Beta-defensin-1-2-3与食管贲门双源癌密切相关,为食管贲门双源癌肿瘤标志筛选提供重要线索。OBJECTIVE：To establish the proteomic model for primary concurrent cancer of the esophagus and gastric cardia from the same patient （CC） and to identify the biomarkers associated with CC through proteomic analysis on serum from CC pa tients and healthy controls. METHODS： ELDI-TOF-MS methods were applied to serum samples from CC patientss （n= 19） and healthy control （n=50）. Candidate proteins and genes were detected by SWISS-PROT and RT-PCR. RESULIS： Six tumor markers （2. 866 21 × 10^3 , 5. 103 30× 10^3, 6. 597 65 × 10^3 , 7. 931 55× 10^3 , 9. 311 96× 10^3 and 4. 113 99×10^3 ） were identified to discriminate the patients with CC and healthy control with a veracity, sensitivity and specialty of 78. 26%, 73. 68% and 80% respectively. The proteins of 5 340. 52Da and 5 921.32Da were identified as COX7c and Beta-defensin-1-2 3. The positive rates were 60%（3/5）, 60%（3/5） and 60%（3/5）, 40%（2/5） in esophageal carcinoma and gastric cardia adenocarcinonm in CC pa tients respectively. The positive rates were zero in normal esophageal and gastric cardia tissues in CC patients respectively. CON- CI,USION： The diagnosis model with six protein markers of 2. 866 21 ×10^3 , 5. 103 30 × 10^3 , 6, 597 65 × 10^3 , 7. 931 55 × 10^3, 9. 311 96×10^3 and 4. 113 99× 10^3 has a higher sensitivity and specificity for CC. The proteins of COX7c and Beta-defensin 1 2 3 may be related to CC, which provide important clues for identifying tumor markers for CC.

关 键 词：肿瘤 多原发性 贲门 蛋白质组学 肿瘤标记 生物学 光谱法 质量 基质辅助激光解吸电离 

分 类 号：R735[医药卫生—肿瘤]