致癌基因诱导的衰老通路中的种系突变与多个息肉状锯齿状腺瘤有关。
Germline mutations in oncogene-induced senescence pathways are associated with multiple sessile serrated adenomas.
出版信息
Gastroenterology. 2014 Feb;146(2):520-9. doi: 10.1053/j.gastro.2013.10.045.
BACKGROUND & AIMS: Little is known about the genetic factors that contribute to the development of sessile serrated adenomas (SSAs). SSAs contain somatic mutations in BRAF or KRAS early in development. However, evidence from humans and mouse models indicates that these mutations result in oncogene-induced senescence (OIS) of intestinal crypt cells. Progression to serrated neoplasia requires cells to escape OIS via inactivation of tumor suppressor pathways. We investigated whether subjects with multiple SSAs carry germline loss-of function mutations (nonsense and splice site) in genes that regulate OIS: the p16-Rb and ATM-ATR DNA damage response pathways.
METHODS
Through a bioinformatic analysis of the literature, we identified a set of genes that function at the main nodes of the p16-Rb and ATM-ATR DNA damage response pathways. We performed whole-exome sequencing of 20 unrelated subjects with multiple SSAs; most had features of serrated polyposis. We compared sequences with those from 4300 subjects matched for ethnicity (controls). We also used an integrative genomics approach to identify additional genes involved in senescence mechanisms.
RESULTS
We identified mutations in genes that regulate senescence (ATM, PIF1, TELO2,XAF1, and RBL1) in 5 of 20 subjects with multiple SSAs (odds ratio, 3.0; 95% confidence interval, 0.9–8.9; P =.04). In 2 subjects,we found nonsense mutations in RNF43, indicating that it is also associated with multiple serrated polyps (odds ratio, 460; 95% confidence interval, 23.1–16,384; P = 6.8 x 10(-5)). In knockdown experiments with pancreatic duct cells exposed to UV light, RNF43 appeared to function as a regulator of ATMATRDNA damage response.
CONCLUSIONS
We associated germline loss-of-function variants in genes that regulate senescence pathways with the development of multiple SSAs.We identified RNF43 as a regulator of the DNA damage response and associated nonsense variants in this gene with a high risk of developing SSAs.
背景与目的
关于导致无蒂锯齿状腺瘤(SSA)发展的遗传因素知之甚少。SSA 在早期发育时含有 BRAF 或 KRAS 的体细胞突变。然而,来自人类和小鼠模型的证据表明,这些突变导致肠隐窝细胞的癌基因诱导的衰老(OIS)。向锯齿状肿瘤的进展需要细胞通过失活肿瘤抑制途径来逃避 OIS。我们研究了是否具有多个 SSA 的受试者携带调节 OIS 的基因(p16-Rb 和 ATM-ATR DNA 损伤反应途径)的种系失活功能突变(无义和剪接位点)。
方法
通过对文献的生物信息学分析,我们确定了一组在 p16-Rb 和 ATM-ATR DNA 损伤反应途径的主要节点起作用的基因。我们对 20 名无蒂锯齿状腺瘤患者进行了全外显子组测序;大多数具有锯齿状息肉病的特征。我们将序列与 4300 名匹配种族的受试者(对照组)的序列进行比较。我们还使用整合基因组学方法来鉴定参与衰老机制的其他基因。
结果
我们在 20 名具有多个 SSA 的受试者中发现了调节衰老的基因(ATM、PIF1、TELO2、XAF1 和 RBL1)中的突变(比值比,3.0;95%置信区间,0.9–8.9;P =.04)。在 2 名受试者中,我们发现 RNF43 中的无义突变,表明它也与多个锯齿状息肉有关(比值比,460;95%置信区间,23.1–16384;P = 6.8 x 10(-5))。在暴露于紫外线的胰腺导管细胞的敲低实验中,RNF43 似乎作为 ATM-ATR DNA 损伤反应的调节剂发挥作用。
结论
我们将调节衰老途径的基因中的种系失活功能变体与多个 SSA 的发展联系起来。我们确定 RNF43 是 DNA 损伤反应的调节剂,并确定该基因中的无义变异与 SSA 的高风险相关。
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