Epigenomic profiling of primary gastric adenocarcinoma reveals super-enhancer heterogeneity

نویسندگان

  • Wen Fong Ooi
  • Manjie Xing
  • Chang Xu
  • Xiaosai Yao
  • Muhammad Khairul Ramlee
  • Mei Chee Lim
  • Fan Cao
  • Kevin Lim
  • Deepak Babu
  • Lai-Fong Poon
  • Joyce Lin Suling
  • Aditi Qamra
  • Astrid Irwanto
  • James Qu Zhengzhong
  • Tannistha Nandi
  • Ai Ping Lee-Lim
  • Yang Sun Chan
  • Su Ting Tay
  • Ming Hui Lee
  • James O J Davies
  • Wai Keong Wong
  • Khee Chee Soo
  • Weng Hoong Chan
  • Hock Soo Ong
  • Pierce Chow
  • Chow Yin Wong
  • Sun Young Rha
  • Jianjun Liu
  • Axel M Hillmer
  • Jim R Hughes
  • Steve Rozen
  • Bin Tean Teh
  • Melissa Jane Fullwood
  • Shang Li
  • Patrick Tan
چکیده

Regulatory enhancer elements in solid tumours remain poorly characterized. Here we apply micro-scale chromatin profiling to survey the distal enhancer landscape of primary gastric adenocarcinoma (GC), a leading cause of global cancer mortality. Integrating 110 epigenomic profiles from primary GCs, normal gastric tissues and cell lines, we highlight 36,973 predicted enhancers and 3,759 predicted super-enhancers respectively. Cell-line-defined super-enhancers can be subclassified by their somatic alteration status into somatic gain, loss and unaltered categories, each displaying distinct epigenetic, transcriptional and pathway enrichments. Somatic gain super-enhancers are associated with complex chromatin interaction profiles, expression patterns correlated with patient outcome and dense co-occupancy of the transcription factors CDX2 and HNF4α. Somatic super-enhancers are also enriched in genetic risk SNPs associated with cancer predisposition. Our results reveal a genome-wide reprogramming of the GC enhancer and super-enhancer landscape during tumorigenesis, contributing to dysregulated local and regional cancer gene expression.

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عنوان ژورنال:

دوره 7  شماره 

صفحات  -

تاریخ انتشار 2016