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胃癌及周围肠上皮化生黏膜中分子改变的研究:孤立腺分析。

Molecular alterations in gastric cancer and the surrounding intestinal metaplastic mucosa: an analysis of isolated glands.

机构信息

Department of Molecular Diagnostic Pathology, School of Medicine, Iwate Medical University, 2-1-1, Shiwa, Yahaba, Morioka, 028-3695, Japan.

Department of Pharmacodynamics and Molecular Genetics, School of Pharmacy, Iwate Medical University, 2-1-1, Shiwa, Yahaba, Morioka, 028-3695, Japan.

出版信息

Gastric Cancer. 2021 Mar;24(2):382-391. doi: 10.1007/s10120-020-01130-z. Epub 2020 Nov 3.

Abstract

BACKGROUND

Intestinal metaplasias (IMs) are generally regarded as pre-neoplastic gastric lesions. However, molecular alterations including genetic and epigenetic changes occurring in individual IM glands are not well defined.

AIMS

We sought to identify DNA methylation status, microsatellite instability (MSI) and allelic imbalance (AI) occurring in individual IM glands and non-IM glands within the same mucosa.

METHODS

We divided examined isolated gland obtained from GC into 4 components: isolated cancer, antral isolated intestinal metaplastic tissue, antral isolated non-metaplastic gland and isolated non-metaplastic gland derived from the greater curvature of the most distant gastric body without mucosal atrophy. We examined AI and microsatellite instability statuses using PCR-based microsatellite analysis. Next, the DNA methylation status (high methylation epigenome [HME], intermediate methylation epigenome [IME], and low methylation epigenome [LME]) was investigated. DNA methylation analysis of CDKN2A, mir34-b/c and MLHI genes was also performed.

RESULTS

Although antral isolated IM glands were characterized by IME, isolated non-IM glands showed LME. In isolated cancer glands, HME was frequently found, compared with isolated non-IM glands. DNA methylation of mir34-b/c was common in isolated cancer and IM glands, whereas DNA methylation of CDKN2A was a rare event in isolated samples. The MLH1 gene was not methylated in isolated non-IM glands. Although multiple AIs were frequently found in isolated cancer glands, a few AIs were detected in isolated IM glands.

CONCLUSIONS

We suggest that the DNA methylation status and the status of the mir34-b/c gene among isolated samples of IMs and isolated non-IM glands have an impact on IM development.

摘要

背景

肠上皮化生(IMs)通常被认为是癌前胃病变。然而,在个别 IM 腺体中发生的分子改变,包括遗传和表观遗传改变,尚未得到很好的定义。

目的

我们旨在确定在同一黏膜内的单个 IM 腺体和非 IM 腺体中发生的 DNA 甲基化状态、微卫星不稳定性(MSI)和等位基因失衡(AI)。

方法

我们将从 GC 中分离出的单个腺体分为 4 个成分:孤立的癌、胃窦部分离的肠上皮化生组织、胃窦部分离的非化生腺体和来自胃体最远端大弯侧、无黏膜萎缩的分离的非化生腺体。我们使用基于 PCR 的微卫星分析来检查 AI 和微卫星不稳定性状态。接下来,我们研究了 DNA 甲基化状态(高甲基化表观基因组[HME]、中间甲基化表观基因组[IME]和低甲基化表观基因组[LME])。还进行了 CDKN2A、mir34-b/c 和 MLHI 基因的 DNA 甲基化分析。

结果

尽管胃窦部分离的 IM 腺体的特征是 IME,但分离的非 IM 腺体显示 LME。与分离的非 IM 腺体相比,在分离的癌腺体中经常发现 HME。mir34-b/c 的 DNA 甲基化在分离的癌和 IM 腺体中很常见,而 CDKN2A 的 DNA 甲基化在分离的样本中是罕见事件。MLH1 基因在分离的非 IM 腺体中未甲基化。尽管在分离的癌腺体中经常发现多个 AI,但在分离的 IM 腺体中仅检测到少数 AI。

结论

我们认为 IM 和分离的非 IM 腺体中分离样本的 DNA 甲基化状态和 mir34-b/c 基因状态对 IM 的发展有影响。

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