You Jeong Heo, Soomin Ahn, So Young Kang, Hyunjin Kim, Byung-Hoon Min, Kyoung-Mee Kim
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In conclusion, non-tumor mucosa at 1 cm and 3 cm from the tumor harbored different genomic, transcriptomic, and immune cell profiles. The non-tumor mucosa closer to the tumor (1 cm) exhibited similar genomic and transcriptomic features. 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引用次数: 0
摘要
在早期胃癌中,局部复发发生在内镜下野癌切除后。了解癌症易发环境的性质对于制定有效的预防复发策略非常重要。我们假设非肿瘤(易发癌)组织的分子/免疫谱根据与胃肿瘤的相对距离而不同。为此,我们对16个早期胃癌样本进行了全外显子组和转录组测序,配对的非肿瘤粘膜距离肿瘤1 cm (N1)和3 cm (N3)。全外显子组测序显示肿瘤和非肿瘤粘膜均有突变。TTN是肿瘤中最常改变的基因(31 %),是N1样本中第二常改变的基因(25 %);而N3样品的突变率较低,为12 % (P = 0.0046)。此外,TTN mRNA在肿瘤中的表达水平高于N1和N3样品,并与TTN突变显著相关(P = 0.04)。TP53突变主要发生在肿瘤(50 %)和6.3 %的N1中,在N3样本中未检测到突变。转录组测序显示,肿瘤组织中上皮-间充质转化信号、间充质信号和增殖信号的表达增加,而非肿瘤组织中程序性死亡配体1的表达减少。在肿瘤中,虽然M0/M1巨噬细胞、中性粒细胞和嗜酸性粒细胞数量增加,但浆细胞数量明显低于非肿瘤粘膜。总之,距离肿瘤1 cm和3 cm的非肿瘤粘膜具有不同的基因组、转录组学和免疫细胞谱。离肿瘤较近的非肿瘤粘膜(1 cm)表现出相似的基因组和转录组特征。这些结果可为早期胃癌内镜切除中获得安全的水平切缘提供临床指导。
Distinct genomic, transcriptomic, and immune profiles for tumor and non-tumor mucosal regions in early gastric cancer.
In early gastric cancer, local recurrence develops after endoscopic resection by field cancerization. Understanding the nature of cancer-prone environments is important to establish effective strategies to prevent recurrence. We hypothesized that the molecular/immune profiles in non-tumor (cancer-prone) tissue differ according to the relative distance from the gastric tumor. For this purpose, we performed whole-exome and transcriptome sequencing of 16 early gastric cancer samples with paired non-tumor mucosa 1 cm (N1) and 3 cm (N3) away from the tumor. The whole exome sequencing revealed mutations in both the tumor and non-tumor mucosa. TTN was the most frequently altered gene in tumors (31 %) and was the second most frequently altered gene in N1 (25 %) samples; however, the mutation rate was significantly lower in N3 (12 %) samples (P = 0.0046). Moreover, the expression levels of TTN mRNA were higher in tumors than in the N1 and N3 samples and were significantly associated with TTN mutations (P = 0.04). TP53 mutations were mainly observed in tumors (50 %) and in 6.3 % of N1, with no mutation detected in N3 samples. Transcriptome sequencing revealed that the expression of the epithelial-mesenchymal transition signature, mesenchymal signature, and proliferation signature was increased in tumors, whereas programmed death-ligand 1 expression was decreased in the non-tumor mucosa. In the tumor, although the numbers of M0/M1 macrophages, neutrophils, and eosinophils increased, plasma cell numbers were markedly decreased compared to non-tumor mucosa. In conclusion, non-tumor mucosa at 1 cm and 3 cm from the tumor harbored different genomic, transcriptomic, and immune cell profiles. The non-tumor mucosa closer to the tumor (1 cm) exhibited similar genomic and transcriptomic features. These findings can offer clinical guidance for acquiring a safe horizontal margin in endoscopic resection for early gastric cancer.
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Pathology, Research and Practice provides accessible coverage of the most recent developments across the entire field of pathology: Reviews focus on recent progress in pathology, while Comments look at interesting current problems and at hypotheses for future developments in pathology. Original Papers present novel findings on all aspects of general, anatomic and molecular pathology. Rapid Communications inform readers on preliminary findings that may be relevant for further studies and need to be communicated quickly. Teaching Cases look at new aspects or special diagnostic problems of diseases and at case reports relevant for the pathologist''s practice.
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