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Genomic landscape of epithelium with low-grade atypia on gastric cancer after Helicobacter pylori eradiation therapy

Authors
  • Masuda, Kazuhiko1
  • Urabe, Yuji1, 2, 3
  • Ito, Masanori1
  • Ono, Atsushi1, 3
  • Clair Nelson, Hayes1, 3
  • Nakamura, Koki1
  • Kotachi, Takahiro2
  • Boda, Tomoyuki2
  • Tanaka, Shinji2
  • Chayama, Kazuaki1, 3
  • 1 Hiroshima University, 1-2-3 Kasumi, Minami-ku, Hiroshima, 734-8551, Japan , Hiroshima (Japan)
  • 2 Hiroshima University Hospital, Hiroshima, Japan , Hiroshima (Japan)
  • 3 Hiroshima University, Hiroshima, Japan , Hiroshima (Japan)
Type
Published Article
Journal
Journal of Gastroenterology
Publisher
Springer Singapore
Publication Date
Jun 13, 2019
Volume
54
Issue
10
Pages
907–915
Identifiers
DOI: 10.1007/s00535-019-01596-4
Source
Springer Nature
Keywords
License
Green

Abstract

BackgroundGastric cancer may develop after successful eradication of Helicobacter pylori, although the incidence is lower than in non-eradicated individuals. We previously reported the appearance of characteristic epithelium with low-grade atypia (ELA) on the surface of gastric cancer after H. pylori eradication. However, whether ELA originates from cancer after re-differentiation or from the non-cancerous surrounding mucosa is unknown.MethodsWe isolated ELA regions from 10 early gastric cancer patients and analyzed the nucleotide sequences for 90 oncogenes and 35 fusion oncogenes, comparing them with counterpart cancer tissue, normal gastric mucosa, and blood cell-derived DNA. Somatic mutations in each tissue were identified by comparing them with the sequences from whole blood-derived DNA.ResultGene alterations were observed in nine of the ten patients, and up to 42 and 70 somatic mutations were seen in cancer and ELA samples, respectively. Common mutations shared between cancer and ELA tissues were found in eight of these nine patients. In contrast, common mutations between non-cancer mucosa and ELA were only detected in one patient, who also had common mutation between cancer and ELA. ELA-specific nucleotide substitutions were seen in seven patients. In contrast, cancer-specific substitutions were only found in two patients. 18 out of 19 amino acid substitutions present in cancer tissue were also identified in ELA. These results suggest that ELA originated from cancer tissue and accumulated further nucleotide substitutions.ConclusionsDifferential diagnosis of ELA and normal mucosa should be carefully performed to prevent misdiagnosis of ELA as normal mucosa with atypia.

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