Division of Molecular and Diagnostic Pathology, Department of Pathology, Shiga University of Medical Science, Ōtsu, Japan.
Department of Pathology, Ho Chi Minh City University of Medicine and Pharmacy, Ho Chi Minh City, Vietnam.
Pathobiology. 2019;86(2-3):118-127. doi: 10.1159/000494926. Epub 2019 Jan 9.
To examine whether gastric carcinoma (GC) with chromosomal instability (CIN-type GC), the largest category in the Cancer Genome Atlas classification, consists of a single genetic lineage, we conducted a multisampling analysis of genomic DNA copy-number profile.
We performed array-based comparative genomic hybridization using formalin-fixed paraffin-embedded tissues from 54 gland-forming GCs containing a total of 106 DNA samples from mucosal, extramucosal invasive, and lymph node lesions. Microarray data were analyzed by unsupervised hierarchical clustering and penetrance plots. Epstein-Barr virus infection status and mismatch repair (MMR) enzyme-silencing/p53/mucin expression were examined by in situ hybridization and immunohistochemistry, respectively.
The samples examined were divided into gain-rich cluster A and loss-rich cluster B, which were different in tumor locus and patient age. The T1/T2-4 ratio, the frequency of small cancers (diameter ≤2-4 cm), and
We demonstrated that CIN-type GC could be categorized into 2 genetic lineages which are different in terms of rapidity of local extension but similar in terms of nodal metastasis risk.
为了研究染色体不稳定性(CIN 型 GC)是否为癌症基因组图谱分类中最大的一类胃癌(GC),由单一遗传谱系组成,我们对基因组 DNA 拷贝数谱进行了多采样分析。
我们使用福尔马林固定石蜡包埋组织进行基于阵列的比较基因组杂交,这些组织来自 54 个具有腺体形成的 GC,总共包含来自黏膜、黏膜外浸润和淋巴结病变的 106 个 DNA 样本。通过无监督层次聚类和渗透图分析微阵列数据。通过原位杂交和免疫组织化学分别检查 Epstein-Barr 病毒感染状态和错配修复(MMR)酶沉默/p53/粘蛋白表达。
所检查的样本分为富含增益的簇 A 和富含缺失的簇 B,它们在肿瘤部位和患者年龄上存在差异。簇 B 的 T1/T2-4 比、小癌症(直径≤2-4cm)的频率和<下划线></下划线>肠粘蛋白表达均高于簇 A,但簇 A 和簇 B 之间 MMR 沉默、突变 p53 模式和淋巴结转移的频率没有显著差异。
我们证明 CIN 型 GC 可以分为 2 种遗传谱系,它们在局部扩展的速度上有所不同,但在淋巴结转移风险方面相似。
