Details

Autor(en) / Beteiligte

• Cheng, Alfred S.L
• Li, May S
• Kang, Wei
• Cheng, Victoria Y
• Chou, Jian–Liang
• Lau, Suki S
• Go, Minnie Y
• Lee, Ching C
• Ling, Thomas K
• Ng, Enders K
• Yu, Jun
• Huang, Tim H
• To, Ka F
• Chan, Michael W
• Sung, Joseph J.Y
• Chan, Francis K.L

Titel

Helicobacter pylori Causes Epigenetic Dysregulation of FOXD3 to Promote Gastric Carcinogenesis

Ist Teil von

• Gastroenterology (New York, N.Y. 1943), 2013, Vol.144 (1), p.122-133.e9

Ort / Verlag

United States: Elsevier Inc

Erscheinungsjahr

2013

Quelle

MEDLINE

Beschreibungen/Notizen

• Background & Aims Deregulation of forkhead box (Fox) proteins, an evolutionarily conserved family of transcriptional regulators, leads to tumorigenesis. Little is known about their regulation or functions in the pathogenesis of gastric cancer. Promoter hypermethylation occurs during Helicobacter pylori –induced gastritis. We investigated whether the deregulated genes contribute to gastric tumorigenesis. Methods We used integrative genome-wide scans to identify concomitant hypermethylated genes in mice infected with H pylori and human gastric cancer samples. We also analyzed epigenetic gene silencing in gastric tissues from patients with H pylori infection and gastritis, intestinal metaplasia, gastric tumors, or without disease (controls). Target genes were identified by chromatin immunoprecipitation microarrays and expression and luciferase reporter analyses. Results Methylation profile analyses identified the promoter of FOXD3 as the only genomic region with increased methylation in mice and humans during progression of H pylori –associated gastric tumors. FOXD3 methylation also correlated with shorter survival times of patients with gastric cancer. Genome demethylation reactivated FOXD3 expression in gastric cancer cell lines. Transgenic overexpression of FOXD3 significantly inhibited gastric cancer cell proliferation and invasion, and reduced growth of xenograft tumors in mice, at least partially, by promoting tumor cell apoptosis. FOXD3 bound directly to the promoters of, and activated transcription of, genes encoding the cell death regulators CYFIP2 and RARB. Levels of FOXD3 , CYFIP2, and RARB messenger RNAs were reduced in human gastric tumor samples, compared with control tissues. Conclusions FOXD3-mediated transcriptional control of tumor suppressors is deregulated by H pylori infection–induced hypermethylation; this could perturb the balance between cell death and survival. These findings identify a pathway by which epigenetic changes affect gastric tumor suppression.