Sequence of molecular genetic events in colorectal tumorigenesis.

Pierre Laurent-Puig, H. Bons, P. Cugnenc
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引用次数: 74

Abstract

Intensive screening for genetic alteration in colorectal cancer led to the identification of two types of colorectal tumours that are distinct by their carcinogenesis processes. The first group, named LOH (for loss of heterozygosity)-positive, is characterized by hyperploidy and allelic losses involving preferentially chromosome 18q and chromosome 17p. More than two-thirds of colorectal cancers belong to this group. The second group, called multiple microsatellite loci (MSI)-positive cancers, is characterized by genetic instability at microsatellite loci. Although colorectal cancer cells are characterized by specific microsatellite alterations, the same four different signalling pathways, WNT/Wingless pathway, K-ras pathway, transforming growth factor (TGF)beta pathway and p53 pathway, could be implicated in tumour progression. The WNT/Wingless pathway could be altered in two different ways according to whether the cancer cells belong to the group of LOH-positive or MSI-positive tumours. LOH-positive tumours activate the WNT/Wingless signalling pathway through an adenomatous polyposis coli (APC) mutation, whereas the MSI-positive tumours activate this pathway through a beta-catenin stabilizing mutation. Beta-catenin and APC mutations were observed as early as the adenomatous stage of colorectal neoplasia. In TGFbeta pathways LOH-positive tumours inactivated SMAD2 (similar to mother against decapentaplegic drosophilia) or SMAD4, whereas in MSI-positive tumours the TGFbeta type II receptor is frequently deleted. Alteration of these genes correlated closely with the progression of the adenoma to cancer. In the p53 pathway LOH-positive tumours showed frequent p53 mutation, whereas MSI-positive tumours demonstrated BAX (BCL-2-associated X protein)-inactivating mutation. These alterations contribute to the adenoma-carcinoma transition.
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结直肠肿瘤发生的分子遗传事件序列。
对结直肠癌基因改变的密集筛查导致鉴定出两种类型的结直肠癌肿瘤,它们的致癌过程是不同的。第一组被称为LOH(杂合性缺失)阳性,其特征是高倍性和等位基因丢失,优先涉及18q染色体和17p染色体。超过三分之二的结直肠癌属于这一群体。第二组称为多微卫星位点(MSI)阳性癌症,其特征是微卫星位点的遗传不稳定。尽管结直肠癌细胞具有特异性微卫星改变的特征,但同样的四种不同的信号通路,即WNT/无翼通路、K-ras通路、转化生长因子(TGF) β通路和p53通路,可能与肿瘤进展有关。根据癌细胞属于loh阳性组还是msi阳性组,WNT/Wingless通路可以通过两种不同的方式改变。loh阳性肿瘤通过腺瘤性息肉病大肠杆菌(APC)突变激活WNT/无翼信号通路,而msi阳性肿瘤通过β -连环蛋白稳定突变激活该通路。β -连环蛋白和APC突变早在结直肠肿瘤腺瘤期就被观察到。在tgf β途径中,loh阳性肿瘤灭活SMAD2(类似于母亲抗十肢截瘫果蝇)或SMAD4,而在msi阳性肿瘤中,tgf β II型受体经常被删除。这些基因的改变与腺瘤向癌症的进展密切相关。在p53通路中,loh阳性肿瘤显示p53频繁突变,而msi阳性肿瘤显示BAX (bcl -2相关X蛋白)失活突变。这些改变有助于腺瘤向癌的转变。
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