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首页> 外文期刊>British Journal of Cancer >Contrasting molecular pathology of colorectal carcinoma in Egyptian and Western patients
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Contrasting molecular pathology of colorectal carcinoma in Egyptian and Western patients

机译:埃及和西方患者大肠癌的分子病理学对比

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Colorectal carcinoma is uncommon in Egypt, but a high proportion of cases occurs before age 40 years and in the rectum. We compared the molecular pathology of 59 representative Egyptian patients aged 10–72 to Western patients with sporadic, young-onset, or hereditary non-polyposis colorectal cancer syndrome (HNPCC)-associated carcinoma and found significant differences. Most Egyptian cancers were rectal (51%) and poorly differentiated (58%). High levels of microsatellite instability (MSI-H) were frequent (37%) and attributable in some cases (36%) to methylation of the promoter of the hMLH1 mismatch repair gene, but no MSI-H cancer had loss of hMSH2 mismatch repair gene product of the type seen with germline hMSH2 mutation in HNPCC. K-ras mutation was uncommon (11%). In subset analyses, high frequencies of MSI-H in rectal carcinomas (36%) and p53 gene product overexpression in MSI-H cancers (50%) were found. MSI-H and K-ras mutation in Egyptians under age 40 were unusual (17% and 0%, respectively), and schistosomiasis was associated with MSI and K-ras mutation. Cluster analysis identified 2 groups: predominantly young men with poorly differentiated mucinous and signet-ring cell colorectal carcinoma lacking K-ras mutation; older patients who had well- or moderately differentiated adenocarcinoma often with MSI-H, K-ras mutation and schistosomiasis. Our findings show that the molecular pathology of colorectal cancer in older as well as younger Egyptians has unique differences from Western patients, and schistosomiasis influences the molecular pathogenesis of some tumours. ? 2001 Cancer Research Campaign http://www.bjcancer.com
机译:结直肠癌在埃及并不常见,但很大一部分病例发生在40岁之前和直肠中。我们比较了59例年龄在10-72岁的埃及代表性患者与西方散发,年轻发作或遗传性非息肉性大肠直肠癌综合征(HNPCC)相关的癌症患者的分子病理学,发现有显着差异。大部分埃及癌症为直肠癌(51%),分化差(58%)。高水平的微卫星不稳定性(MSI-H)频繁(37%),在某些情况下(36%)可归因于hMLH1错配修复基因启动子的甲基化,但没有MSI-H癌症的hMSH2错配丢失HNPCC中带有种系hMSH2突变的修复基因产物。 K-ras突变并不常见(11%)。在子集分析中,发现直肠癌中MSI-H的频率很高(36%),MSI-H癌症中的p53基因产物过表达(50%)。 40岁以下埃及人的MSI-H和K-ras突变异常(分别为17%和0%),血吸虫病与MSI和K-ras突变相关。聚类分析确定了两组:主要是年轻人,他们的粘液性和印戒细胞大肠癌分化较差,缺乏K-ras突变;患有高分化或中度分化腺癌的老年患者常伴有MSI-H,K-ras突变和血吸虫病。我们的发现表明,年龄较大的埃及人和年轻人的结直肠癌的分子病理学与西方患者具有独特的差异,而血吸虫病会影响某些肿瘤的分子发病机理。 ? 2001年癌症研究运动http://www.bjcancer.com

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