以色列不同种族散发性结直肠癌的微卫星不稳定性、MLH1启动子甲基化及BRAF突变分析
Microsatellite instability, MLH1 promoter methylation, and BRAF mutation analysis in sporadic colorectal cancers of different ethnic groups in Israel.
作者信息
Vilkin Alex, Niv Yaron, Nagasaka Takeshi, Morgenstern Sarah, Levi Zohar, Fireman Zvi, Fuerst Florentine, Goel Ajay, Boland C Richard
机构信息
Department of Gastroenterology, Rabin Medical Center, Beilinson Hospital, Tel Aviv University, Tel Aviv, Israel.
出版信息
Cancer. 2009 Feb 15;115(4):760-9. doi: 10.1002/cncr.24019.
BACKGROUND
The molecular mechanisms that underlie colorectal cancer (CRC) include microsatellite instability (MSI), chromosomal instability, and the CpG island methylator phenotype. There is evidence to suggest that CRC incidence varies among different ethnic populations worldwide. The authors of this report hypothesized that environmental factors and lifestyle differences among various ethnic groups may differentially influence the epigenetic regulation of tumor suppressor genes in CRC.
METHODS
In the current study, microdissection and DNA extraction were performed on 128 samples of CRC from Israeli patients (85 Jews and 43 Arabs). MSI analysis, mutL homolog 1 (MLH1) and mutS homolog 2 (MSH2) protein expression levels, and MLH1 promoter methylation were investigated by combined bisulfite restriction analysis. The v-raf murine sarcoma viral oncogene homolog B1 (BRAF) valine-to-glutamic acid mutation at residue 600 was investigated by direct DNA sequencing.
RESULTS
High MSI (MSI-H), MLH1 methylation, and BRAF mutations were observed in 11.6%, 9.4%, and 23.5% of Jews, respectively, and in 16.2%, 17.6%, and 20.9% of Arabs, respectively (P value nonsignificant). MLH1 promoter methylation was observed in 22.6% of microsatellite-stable (MSS) tumors and in 53.8% of MSI-H tumors (P < .015). Extensive methylation (covering both 5' and 3' promoter regions) was present in all MSI-H tumors with loss of MLH1 expression. BRAF mutation was observed in 15.6% and 46.1% of MSS tumors and MSI-H tumors, respectively (P < .007). BRAF mutation was observed in 66%, 22.2%, and 14.7% of patients who had tumors with extensive MLH1 promoter methylation, methylation of the 5' region alone, or without methylation, respectively (P < .006).
CONCLUSIONS
There was no difference in molecular signatures examined between Jewish and Arab patients with CRC in Israel. Extensive promoter methylation was associated with MLH1 inactivation, MSI, and BRAF mutation.
背景
结直肠癌(CRC)的分子机制包括微卫星不稳定性(MSI)、染色体不稳定性和CpG岛甲基化表型。有证据表明,全球不同种族人群的结直肠癌发病率存在差异。本报告的作者推测,不同种族群体之间的环境因素和生活方式差异可能对结直肠癌中抑癌基因的表观遗传调控产生不同影响。
方法
在本研究中,对128例来自以色列患者(85名犹太人和43名阿拉伯人)的结直肠癌样本进行了显微切割和DNA提取。通过联合亚硫酸氢盐限制性分析研究了MSI分析、错配修复蛋白mutL同源物1(MLH1)和错配修复蛋白mutS同源物2(MSH2)的蛋白表达水平以及MLH1启动子甲基化情况。通过直接DNA测序研究了第600位密码子处v-raf鼠肉瘤病毒癌基因同源物B1(BRAF)缬氨酸到谷氨酸的突变情况。
结果
在犹太患者中,分别有11.6%、9.4%和23.5%的患者观察到高微卫星不稳定性(MSI-H)、MLH1甲基化和BRAF突变;在阿拉伯患者中,相应比例分别为16.2%、17.6%和20.9%(P值无统计学意义)。在22.6%的微卫星稳定(MSS)肿瘤和53.8%的MSI-H肿瘤中观察到MLH1启动子甲基化(P <.015)。在所有MLH1表达缺失的MSI-H肿瘤中均存在广泛甲基化(覆盖5'和3'启动子区域)。在MSS肿瘤和MSI-H肿瘤中,BRAF突变的发生率分别为15.6%和46.1%(P <.007)。在MLH1启动子广泛甲基化、仅5'区域甲基化或未甲基化的肿瘤患者中,BRAF突变的发生率分别为66%、22.2%和14.7%(P <.006)。
结论
在以色列,犹太人和阿拉伯结直肠癌患者之间所检测的分子特征没有差异。广泛的启动子甲基化与MLH1失活、MSI和BRAF突变相关。
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