中国北方遗传性非息肉病性结直肠癌人群的微卫星不稳定性和新型错配修复基因突变。

Jian Qiu Sheng, Tsun Leung Chan, Yee Wai Chan, Ji Sheng Huang, Ji Gui Chen, Ming Zhi Zhang, Xiu Lan Guo, Hong Mu, Annie Sy Chan, Shi Rong Li, Siu Tsan Yuen, Suet Yi Leung
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引用次数: 27

摘要

目的:遗传性非息肉病性结直肠癌(HNPCC)综合征是遗传性结直肠癌最常见的病因,发病年龄早。在大多数HNPCC家族中发现了DNA错配修复(MMR)基因之一的微卫星不稳定性(MSI)和种系突变,为遗传诊断和预防性筛查提供了机会。MMR基因突变谱可能在不同的人群中有所不同,并受到特定种族群体中普遍存在的创始突变的影响。中国是一个古老的大国,有着巨大的基因多样性,这在中国北方和南方人口之间尤为明显。先前已经建立了一个以香港为基地的中国南方人口的MMR基因突变数据库。本研究比较了中国北方和南方人群HNPCC的MMR基因突变谱和MSI。方法:对中国北方25个HNPCC家族进行系统分析。MSI分析采用美国国家癌症研究所(NCI)面板中的5个基因座(D2S123, D5S346, BAT-25, BAT-26和BAT-40),通过PCR从肿瘤和正常组织中进行。免疫组织化学染色检测MSH2、MSH6和MLH1。利用MSH2缺失位点(c.1452_1455delAATG)和MLH1外显子11缺失位点1.8 kb的引物,对MSH2和MLH1的两个始祖突变进行PCR碱基分析。结果:在所收集的25个家庭中,19个符合Bethesda指南(BG) 1, 6个符合BG3。22例(15.7%)为结肠癌外癌伴胃癌(7例)是最常见的癌症类型。在分析的25例肿瘤中,21例(84%)为高水平微卫星不稳定(MSI-H), 4例(16%)为微卫星稳定(MSS)。21例MSI-H肿瘤中有18例(86%)显示MLH1或MSH2蛋白缺失。3例MSI-H肿瘤和4例MSS肿瘤均未出现3种MMR蛋白的表达缺失。在21例MSI-H肿瘤患者中,12例(57%)显示MLH1 (n = 8)或MSH2 (n = 4)的致病性种系突变。总体而言,已鉴定出3种新突变(患者H22、H17和H29)。其中的c.503_4insA引起了MLH1基因的移码突变。另外两个在MSH2基因中发现,包括移码(c.899_890insAT)和剪接连接(IVS7-1G- > a, SA的外显子8)突变。结论:结果表明,中国北方和南方人群的MMR基因突变谱明显不同,需要进行系统的、全国性的研究,以促进针对中国个体人群的MMR基因突变检测策略的设计。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Microsatellite instability and novel mismatch repair gene mutations in northern Chinese population with hereditary non-polyposis colorectal cancer.

Objective: Hereditary non-polyposis colorectal cancer (HNPCC) syndrome is the most common cause of hereditary colorectal cancer with an early age of onset. Microsatellite instability (MSI) and germline mutation in one of the DNA mismatch repair (MMR) genes are found in the majority of HNPCC families and provide an opportunity for genetic diagnosis and prophylactic screening. The MMR gene mutation spectrum may vary across different populations and be influenced by founder mutations that prevail in specific ethnic groups. China is a big and ancient nation with enormous genetic diversity, which is especially notable between the northern and southern Chinese populations. A MMR gene mutation database for the southern Chinese population based in Hong Kong has been previously established. This study compares the MMR gene mutation spectrum and the MSI of HNPCC between the northern and southern Chinese populations.

Methods: Twenty-five HNPCC families from northern China were systematically analyzed. The MSI analysis was performed using five loci in the USA National Cancer Institute (NCI) panel (D2S123, D5S346, BAT-25, BAT-26 and BAT-40) by PCR from the tumor and normal tissue. MSH2, MSH6 and MLH1 were performed using immunohistochemical staining. Two founder mutations of MSH2 and MLH1 were examined by PCR base analyses using primers flanking the two deletion sites (c.1452_1455delAATG in MSH2 and 1.8 kb deletion involving exon 11 of MLH1).

Results: Of the 25 families collected, 19 met Bethesda guideline (BG) 1 and six met BG3. Twenty-two (15.7%) were extra-colonic cancers with gastric cancer (in seven patients) being the most common cancer type. Of the 25 tumors analyzed, 21 (84%) were high level microsatellite instability (MSI-H) and four (16%) were microsatellite stable (MSS). Eighteen (86%) of the 21 MSI-H tumors showed loss of either the MLH1 or the MSH2 protein. Three MSI-H tumors and all four MSS tumors showed no loss of expression of the three MMR proteins. Out of the 21 patients with MSI-H tumors, 12 (57%) showed pathogenic germline mutations in either MLH1 (n = 8) or MSH2 (n = 4). Overall, three novel mutations (in patients H22, H17 and H29) have been identified. One of them, c.503_4insA, caused a frameshift mutation in the MLH1 gene. The other two were found in the MSH2 gene, including a frameshift (c.899_890insAT) and a splice junction (IVS7-1G-->A, SA of Exon 8) mutation.

Conclusions: The results suggest a distinctly different mutation spectrum of MMR genes between northern and southern Chinese populations and call for a systematic, nationwide study to facilitate the design of a MMR gene mutation detection strategy tailored for individual populations in China.

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