散发性结肠癌早期进展中DNA修复酶表达不足。

Q4 Biochemistry, Genetics and Molecular Biology

Genome Integrity Pub Date : 2012-04-11 DOI:10.1186/2041-9414-3-3

Alexander Facista, Huy Nguyen, Cristy Lewis, Anil R Prasad, Lois Ramsey, Beryl Zaitlin, Valentine Nfonsam, Robert S Krouse, Harris Bernstein, Claire M Payne, Stephen Stern, Nicole Oatman, Bhaskar Banerjee, Carol Bernstein

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引用次数: 41

摘要

背景:癌症通常发生在易发生癌症的细胞区域(如上皮斑块)，即“癌变场”或“场缺陷”。散发性结肠癌的特点是突变率升高和基因组不稳定。如果场缺陷缺乏DNA修复，DNA损伤将倾向于逃避修复并引起致癌突变。目的:确定DNA修复蛋白Pms2、Ercc1和Xpf (Ercc1的配对伴侣)的表达减少是否在结肠癌进展的早期阶段。结果:对4种不同风险水平的77例结肠癌患者进行结肠镜检查，其中19例从未发生过结肠癌瘤变(对照组)。此外，158个组织样本取自切除的结肠癌附近或内部组织，16个组织样本取自切除的管绒毛腺瘤(tva)附近组织。采用免疫组化方法对568个三重组织切片(共1704个组织切片)进行4种DNA修复蛋白的检测。Pms2、Ercc1和Xpf蛋白表达的显著降低发生在距离结肠癌或tva纵向距离达10 cm的田间缺陷和结肠癌内部。另一种DNA修复蛋白Ku86的表达在这些区域很少减少。当Pms2、Ercc1或Xpf蛋白表达减少时，其他两种蛋白中通常有一种或两种蛋白表达也减少。32例结肠上升区、横区和下降区/乙状结肠平均内周长分别为6.6 cm、5.8 cm和6.3 cm。当与文献中的其他测量相结合时，这表明人类结肠隐窝的平均数量约为1000万个。结论:DNA修复蛋白Pms2、Ercc1和Xpf在肿瘤和tva附近的100万个隐窝中大量缺乏表达，表明肿瘤是由DNA修复缺陷引起的，Pms2、Ercc1和Xpf的缺乏是结肠癌发展的早期阶段，经常同时发生。

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Deficient expression of DNA repair enzymes in early progression to sporadic colon cancer.

Background: Cancers often arise within an area of cells (e.g. an epithelial patch) that is predisposed to the development of cancer, i.e. a "field of cancerization" or "field defect." Sporadic colon cancer is characterized by an elevated mutation rate and genomic instability. If a field defect were deficient in DNA repair, DNA damages would tend to escape repair and give rise to carcinogenic mutations.

Purpose: To determine whether reduced expression of DNA repair proteins Pms2, Ercc1 and Xpf (pairing partner of Ercc1) are early steps in progression to colon cancer.

Results: Tissue biopsies were taken during colonoscopies of 77 patients at 4 different risk levels for colon cancer, including 19 patients who had never had colonic neoplasia (who served as controls). In addition, 158 tissue samples were taken from tissues near or within colon cancers removed by resection and 16 tissue samples were taken near tubulovillous adenomas (TVAs) removed by resection. 568 triplicate tissue sections (a total of 1,704 tissue sections) from these tissue samples were evaluated by immunohistochemistry for 4 DNA repair proteins. Substantially reduced protein expression of Pms2, Ercc1 and Xpf occurred in field defects of up to 10 cm longitudinally distant from colon cancers or TVAs and within colon cancers. Expression of another DNA repair protein, Ku86, was infrequently reduced in these areas. When Pms2, Ercc1 or Xpf were reduced in protein expression, then either one or both of the other two proteins most often had reduced protein expression as well. The mean inner colon circumferences, from 32 resections, of the ascending, transverse and descending/sigmoid areas were measured as 6.6 cm, 5.8 cm and 6.3 cm, respectively. When combined with other measurements in the literature, this indicates the approximate mean number of colonic crypts in humans is 10 million.

Conclusions: The substantial deficiencies in protein expression of DNA repair proteins Pms2, Ercc1 and Xpf in about 1 million crypts near cancers and TVAs suggests that the tumors arose in field defects that were deficient in DNA repair and that deficiencies in Pms2, Ercc1 and Xpf are early steps, often occurring together, in progression to colon cancer.

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Genome Integrity Biochemistry, Genetics and Molecular Biology-Genetics

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