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早期浸润性肺腺癌影像学表现为单纯磨玻璃密度时,组织学边界处及以外的 DNA 甲基化模式。

DNA methylation patterns at and beyond the histological margin of early-stage invasive lung adenocarcinoma radiologically manifested as pure ground-glass opacity.

机构信息

Department of Thoracic Surgery, Peking Union Medical College Hospital, Peking Union Medical College and Chinese Academy of Medical Sciences, Beijing, 100730, China.

Peking Union Medical College, Chinese Academy of Medical Sciences, Beijing, 100730, China.

出版信息

Clin Epigenetics. 2021 Aug 19;13(1):153. doi: 10.1186/s13148-021-01140-3.

Abstract

BACKGROUND

Early-stage lung cancers radiologically manifested as ground-glass opacities (GGOs) have been increasingly identified, among which pure GGO (pGGO) has a good prognosis after local resection. However, the optimal surgical margin is still under debate. Precancerous lesions exist in tumor-adjacent tissues beyond the histological margin. However, potential precancerous epigenetic variation patterns beyond the histological margin of pGGO are yet to be discovered and described.

RESULTS

A genome-wide high-resolution DNA methylation analysis was performed on samples collected from 15 pGGO at tumor core (TC), tumor edge (TE), para-tumor tissues at the 5 mm, 10 mm, 15 mm, 20 mm beyond the tumor, and peripheral normal (PN) tissue. TC and TE were tested with the same genetic alterations, which were also observed in histologically normal tissue at 5 mm in two patients with lower mutation allele frequency. According to the difference of methylation profiles between PN samples, 2284 methylation haplotype blocks (MHBs), 1657 differentially methylated CpG sites (DMCs), and 713 differentially methylated regions (DMRs) were identified using reduced representation bisulfite sequencing (RRBS). Two different patterns of methylation markers were observed: Steep (S) markers sharply changed at 5 mm beyond the histological margin, and Gradual (G) markers changed gradually from TC to PN. S markers composed 86.2% of the tumor-related methylation markers, and G markers composed the other 13.8%. S-marker-associated genes enriched in GO terms that were related to the hallmarks of cancer, and G-markers-associated genes enriched in pathways of stem cell pluripotency and transcriptional misregulation in cancer. Significant difference in DNA methylation score was observed between peripheral normal tissue and tumor-adjacent tissues 5 mm further from the histological margin (p < 0.001 in MHB markers). DNA methylation score at and beyond 10 mm from histological margin is not significantly different from peripheral normal tissues (p > 0.05 in all markers).

CONCLUSIONS

According to the methylation pattern observed in our study, it was implied that methylation alterations were not significantly different between tissues at or beyond P10 and distal normal tissues. This finding explained for the excellent prognosis from radical resections with surgical margins of more than 15 mm. The inclusion of epigenetic characteristics into surgical margin analysis may yield a more sensitive and accurate assessment of remnant cancerous and precancerous cells in the surgical margins.

摘要

背景

越来越多的研究表明,早期肺癌在影像学上表现为磨玻璃密度影(GGO),其中纯磨玻璃密度影(pGGO)在局部切除后预后良好。然而,最佳的手术切缘仍存在争议。肿瘤周围组织存在癌前病变,超出了组织学切缘。然而,pGGO 组织学切缘以外的潜在癌前表观遗传变异模式尚未被发现和描述。

结果

对 15 个 pGGO 的肿瘤核心(TC)、肿瘤边缘(TE)、肿瘤边缘 5mm、10mm、15mm、20mm 处的肿瘤旁组织和外周正常(PN)组织样本进行了全基因组高分辨率 DNA 甲基化分析。TC 和 TE 与两名患者的 5mm 处组织学正常组织中相同的遗传改变进行了检测,这些改变在较低的突变等位基因频率下也被观察到。根据 PN 样本之间甲基化谱的差异,使用简化重亚硫酸盐测序(RRBS)鉴定了 2284 个甲基化单倍型块(MHB)、1657 个差异甲基化 CpG 位点(DMC)和 713 个差异甲基化区域(DMR)。观察到两种不同的甲基化标记模式:陡峭(S)标记在组织学切缘外 5mm 处急剧变化,而渐进(G)标记从 TC 到 PN 逐渐变化。S 标记占肿瘤相关甲基化标记的 86.2%,G 标记占 13.8%。S 标记相关基因在与癌症标志相关的 GO 术语中富集,G 标记相关基因在干细胞多能性和癌症转录失调的途径中富集。在组织学切缘外 5mm 处的外周正常组织和肿瘤旁组织之间观察到 DNA 甲基化评分的显著差异(在 MHB 标记中 p<0.001)。组织学切缘处和 10mm 以外的 DNA 甲基化评分与外周正常组织无显著差异(所有标记中 p>0.05)。

结论

根据我们研究中观察到的甲基化模式,提示组织学切缘处和 10mm 以外的组织之间的甲基化改变无显著差异。这一发现解释了 15mm 以上的根治性切除手术切缘为何能获得良好的预后。将表观遗传学特征纳入手术切缘分析可能会对手术切缘中残留的癌前和癌性细胞进行更敏感和准确的评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1bc9/8375063/d351581d5737/13148_2021_1140_Fig1_HTML.jpg

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