在同时存在结直肠癌的情况下,LINE-1在腺瘤性息肉中优先发生低甲基化。
LINE-1 is preferentially hypomethylated within adenomatous polyps in the presence of synchronous colorectal cancer.
作者信息
Jiang Alice Chu, Buckingham Lela, Barbanera William, Korang Amoah Yeboah, Bishesari Faraz, Melson Joshua
机构信息
Department of Internal Medicine, Rush University Medical Center, 1717 W Congress Parkway, 10 Kellogg, Chicago, IL 60612 USA.
Department of Pathology, Rush University Medical Center, 600 S. Paulina Street, 1014 AAC, Chicago, IL 60612 USA.
出版信息
Clin Epigenetics. 2017 Mar 9;9:25. doi: 10.1186/s13148-017-0325-7. eCollection 2017.
BACKGROUND
Conventional tubular adenomas are frequently detected in patients undergoing average risk screening colonoscopy and are over-represented in patients who will develop colorectal cancer (CRC). Whether features of adenomas could serve as predictors of synchronous CRC is not known. Here, we investigate whether global methylation markers, including LINE-1, differ within adenomas in patients with and without synchronous CRC.
METHODS
Colorectal tubular/tubulovillous adenomatous polyps in the absence (P group, = 45) and in the presence of synchronous CRC (PC group, = 32) were identified. Global methylation and demethylation by ELISA for 5-methylcytosine (5-mC) and 5-hydroxymethyl cytosine (5-hmC), respectively, were assessed in polyps and adjacent normal non-neoplastic tissue. LINE-1 hypomethylation was assessed by pyrosequencing of bisulfite-converted DNA as well.
RESULTS
Global methylation (5-mC) showed no differences in overall methylation status in the adenomatous polyps in the two groups (5-mC relative to control %, PC group 0.117; P group 0.161, = 0.148). Global hydroxymethylation 5-hmC was also not significantly different in adenomatous polyps of the PC group than in those of the P group (0.0059 vs 0.0097, = 0.681). Similarly, global 5-hmC was not different between normal tissues from patients without neoplasia in comparison to those from CRC patients (0.0461 ± 0.080 vs 0.039 ± 0.159, = 0.215). In contrast, adenomatous polyps of the PC group had lower levels of LINE-1 methylation compared to the adenomas in the P group (53.07 ± 4.5 vs 59.95 ± 5.4, < 0.001). LINE-1 methylation was also significantly lower in the normal tissue from cancer patients compared to that from patients without any neoplasia (58.07 ± 3.78 vs 71.50 ± 6.47, < 0.001).
CONCLUSIONS
LINE-1 hypomethylation of precancerous adenomas correlates with the presence of synchronous CRC. Measurement of DNA hypomethylation levels of colorectal adenomas by LINE-1 could have future implications in approaches to defining CRC risk in screening programs.
背景
在进行平均风险筛查结肠镜检查的患者中经常检测到传统管状腺瘤,并且在将发生结直肠癌(CRC)的患者中其比例过高。腺瘤的特征是否可作为同步性CRC的预测指标尚不清楚。在此,我们研究包括LINE-1在内的整体甲基化标志物在有无同步性CRC的患者的腺瘤中是否存在差异。
方法
确定无同步性CRC(P组,n = 45)和有同步性CRC(PC组,n = 32)的结直肠管状/管状绒毛状腺瘤性息肉。分别通过酶联免疫吸附测定法(ELISA)检测息肉及相邻正常非肿瘤组织中5-甲基胞嘧啶(5-mC)和5-羟甲基胞嘧啶(5-hmC)的整体甲基化和去甲基化情况。还通过对亚硫酸氢盐转化的DNA进行焦磷酸测序来评估LINE-1低甲基化情况。
结果
整体甲基化(5-mC)在两组腺瘤性息肉的总体甲基化状态方面无差异(5-mC相对于对照的百分比,PC组0.117;P组0.161,P = 0.148)。PC组腺瘤性息肉中的整体羟甲基化5-hmC与P组相比也无显著差异(0.0059对0.0097,P = 0.681)。同样,与CRC患者的正常组织相比,无肿瘤患者的正常组织之间的整体5-hmC也无差异(0.0461±0.080对0.039±0.159,P = 0.215)。相比之下,PC组的腺瘤性息肉与P组的腺瘤相比,LINE-1甲基化水平较低(53.07±4.5对59.95±5.(此处原文似乎有误,推测可能是5.4),P < 0.001)。与无任何肿瘤的患者的正常组织相比,癌症患者的正常组织中的LINE-1甲基化也显著更低(58.07±3.78对71.50±6.47,P < 0.001)。
结论
癌前腺瘤的LINE-1低甲基化与同步性CRC的存在相关。通过LINE-1测量结直肠腺瘤的DNA低甲基化水平可能对筛查计划中定义CRC风险的方法具有未来意义。
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