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作 者:张放[1] 周崇治[1] 凌云[1] 柏邵春[2] 刘万清[2] 裘国强[1] 贺林[2] 彭志海[1]
机构地区:[1]上海市第一人民医院普外科,200080 [2]中国科学院上海生理学研究所人类分子遗传实验室
出 处:《中华实验外科杂志》2002年第4期320-321,共2页Chinese Journal of Experimental Surgery
基 金:国家自然科学基金资助项目 (30 0 80 0 1 6)
摘 要:目的 探讨散发性结直肠癌患者 18号染色体上抑癌基因相关的杂合缺失 (LOH )情况 ,并探索新的抑癌基因位点。方法 对 83例散发性结直肠癌患者基因组DNA用 14个不同荧光标记的高度多态性微卫星引物 ,扩增相应的微卫星位点 ,平均距离为 10厘摩 (centi morgan ,cM )。用ABIPRISM 3 77测序仪进行基因扫描 ,统计各位点杂合缺失率。结果 在 12个获得有效数据的微卫星位点中 ,平均杂合缺失率为 3 6.78% ,18p中最高为D18S5 3 (3 8.0 9% ) ,18q中最高为D18S474(5 5 .74% )。 4位患者的 18号染色体所有杂合位点都存在缺失 ,3 0位患者的杂合缺失位点不少于 5 0 % (平均 6个 /人 ) ;缺失位点少于 5 0 %的有 5 3人 (平均 1个 /人 )。结论 结直肠癌患者 18号染色体存在高频的LOH ,并以整体缺失为特点。存在高频LOH的区域定位有转化生长因子 (TGF)信号传导相关基因、结直肠癌缺失基因 (DCC)、Rb结合蛋白 8(RbBP8) ,特别是TGF信号传导相关基因MADH 2、4、转化生长因子 β1反应元件 (TGF β1)等的缺失可能对结直肠癌的发生有重要影响。 18p也有存在未知抑癌基因的可能。Objective To study the tumor suppressor gene (TSG) related loss of heterozygosity (LOH) on chromosome 18 in sporadic colorectal cancer.Methods Forteen microsatellite marker primers labeled with 3 different fluorescents were applied to amply the corresponding loci of the genome DNA.The PCR products were electrophoresed on a 377 PRISM sequencer and the fluorescent signals were analyzed by Genotyper and Genescan software.Results The highest LOH ratio was seen at D18S53 (36.67 %) on 18p and at D18S474 (56.14 %) on 18q.There were 4 patients whose markers of chromosome 18 deleted entirely.The percentages of LOH in 30 patients were no less than 50 %,and that of other 53 patients was less than 50 %.Conclusion A highly frequent LOH was found on chromosome 18 in sporadic colorectal cancer patients,which implicated that the deletion of DCC,RBBP8 and TGF signal related genes (MADH2,MADH4 and TGFBRE) might play important roles in the tumorigenesis of colorectal cancer,and that the existence of another unknown TSG on 18p is possible.
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