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BRAF和KRAS基因的突变能够不同程度地区分人类锯齿状与非锯齿状增生异常隐窝灶。

Mutations in BRAF and KRAS differentially distinguish serrated versus non-serrated hyperplastic aberrant crypt foci in humans.

作者信息

Rosenberg Daniel W, Yang Shi, Pleau Devon C, Greenspan Emily J, Stevens Richard G, Rajan Thiruchandurai V, Heinen Christopher D, Levine Joel, Zhou Yijian, O'Brien Michael J

机构信息

Colon Cancer Prevention Program, NEAG Comprehensive Cancer Center, and Center for Molecular Medicine, University of Connecticut Health Center, 263 Farmington Avenue, Farmington, CT 06030, USA.

出版信息

Cancer Res. 2007 Apr 15;67(8):3551-4. doi: 10.1158/0008-5472.CAN-07-0343.

Abstract

We previously reported that colon carcinomas, adenomas, and hyperplastic polyps exhibiting a serrated histology were very likely to possess BRAF mutations, whereas when these same advanced colonic lesions exhibited non-serrated histology, they were wild type for BRAF; among hyperplastic polyps, KRAS mutations were found mainly in a non-serrated variant. On this basis, we predicted that hyperplastic aberrant crypt foci (ACF), a putative precancerous lesion found in the colon, exhibiting a serrated phenotype would also harbor BRAF mutations and that non-serrated ACF would not. In contrast, KRAS mutations would be found more often in the non-serrated ACF. We examined 55 ACF collected during screening colonoscopy from a total of 28 patients. Following laser capture microdissection, DNA was isolated, and mutations in BRAF and KRAS were determined by direct PCR sequencing. When hyperplastic lesions were further classified into serrated and non-serrated histologies, there was a strong inverse relationship between BRAF and KRAS mutations: a BRAF(V600E) mutation was identified in 10 of 16 serrated compared with 1 of 33 non-serrated lesions (P = 0.001); conversely, KRAS mutations were present in 3 of 16 serrated compared with 14 of 33 non-serrated lesions. Our finding of a strong association between BRAF mutations and serrated histology in hyperplastic ACF supports the idea that these lesions are an early, sentinel, or a potentially initiating step on the serrated pathway to colorectal carcinoma.

摘要

我们之前报道过,呈现锯齿状组织学特征的结肠癌、腺瘤和增生性息肉很可能携带BRAF突变,而当这些相同的晚期结肠病变呈现非锯齿状组织学特征时,它们的BRAF为野生型;在增生性息肉中,KRAS突变主要见于非锯齿状变体。在此基础上,我们预测在结肠中发现的一种假定的癌前病变——增生性异常隐窝灶(ACF),若呈现锯齿状表型也会携带BRAF突变,而非锯齿状ACF则不会。相反,KRAS突变在非锯齿状ACF中更常见。我们检查了从总共28名患者的筛查结肠镜检查中收集的55个ACF。经过激光捕获显微切割后,分离出DNA,并通过直接PCR测序确定BRAF和KRAS的突变情况。当增生性病变进一步分为锯齿状和非锯齿状组织学时,BRAF和KRAS突变之间存在强烈的负相关关系:16个锯齿状病变中有10个检测到BRAF(V600E)突变,而33个非锯齿状病变中只有1个(P = 0.001);相反,16个锯齿状病变中有3个存在KRAS突变,而33个非锯齿状病变中有14个存在KRAS突变。我们发现增生性ACF中BRAF突变与锯齿状组织学之间存在强烈关联,这支持了这些病变是结直肠癌锯齿状途径上的早期、哨兵或潜在起始步骤的观点。

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