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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Is early-onset microsatellite and chromosomally stable colorectal cancer a hallmark of a genetic susceptibility syndrome?
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Is early-onset microsatellite and chromosomally stable colorectal cancer a hallmark of a genetic susceptibility syndrome?

机译:早发性微卫星和染色体稳定的结直肠癌是遗传易感综合征的标志吗?

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Most colorectal cancers show either microsatellite or chromosomal instability. A subset of colorectal cancers, especially those diagnosed at young age, is known to show neither of these forms of genetic instability and thus might have a distinct pathogenesis. Colorectal cancers diagnosed at young age are suggestive for hereditary predisposition. We investigate whether such early-onset microsatellite and chromosomally stable colorectal cancers are a hallmark of a genetic susceptibility syndrome. The ploidy status of microsatellite stable (familial) colorectal cancers of patients diagnosed before age 50 (n = 127) was analyzed in relation to the histopathological characteristics and family history. As a control the ploidy status of sporadic colorectal cancer, with normal staining of mismatch repair proteins, diagnosed at the age of 69 years or above (n = 70) was determined. A diploid DNA content was used as a marker for chromosomal stability. Within the group of patients with (familial) early onset microsatellite stable colorectal cancer the chromosomally stable tumors did not differ from chromosomally unstable tumors with respect to mean age at diagnosis, fulfillment of Amsterdam criteria or pathological characteristics. Segregation analysis did not reveal any family with microsatellite and chromosomally stable colorectal cancer in 2 relatives. The prevalence of microsatellite and chromosomally stable colorectal cancer was not significantly different for the early and late onset group (28 and 21%, respectively). We find no evidence that early-onset microsatellite and chromosomally stable colorectal cancer is a hallmark of a hereditary colorectal cancer syndrome.
机译:大多数结直肠癌显示微卫星或染色体不稳定。已知大肠癌的一个子集,尤其是在年轻时诊断出的那些,均未显示出这两种形式的遗传不稳定性,因此可能具有独特的发病机理。在年轻时诊断出的大肠癌可能是遗传性倾向。我们调查这种早期发作的微卫星和染色体稳定的结直肠癌是否是遗传易感性综合征的标志。结合组织病理学特征和家族史,分析了在50岁(n = 127)之前诊断出的患者的微卫星稳定(家族性)结直肠癌的倍性状态。作为对照,确定了散发性结直肠癌的倍性状态,其中错配修复蛋白正常染色,诊断年龄在69岁或以上(n = 70)。二倍体DNA含量用作染色体稳定性的标记。在患有(家族性)早发性微卫星稳定结直肠癌的患者组中,就诊断时的平均年龄,满足阿姆斯特丹标准或病理特征而言,染色体稳定的肿瘤与染色体不稳定的肿瘤没有区别。隔离分析未发现有2个亲属患有微卫星和染色体稳定的结直肠癌。早发和晚发组的微卫星和染色体稳定的结直肠癌的患病率无显着差异(分别为28%和21%)。我们没有证据表明早发性微卫星和染色体稳定的结直肠癌是遗传性结直肠癌综合症的标志。

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