Genome Biology (Nov 2023)

Cooperation of MLL1 and Jun in controlling H3K4me3 on enhancers in colorectal cancer

  • Xiang Lin,
  • Ji-Dong Chen,
  • Chen-Yu Wang,
  • Zhen Cai,
  • Rui Zhan,
  • Chen Yang,
  • La-Ying Zhang,
  • Lian-Yun Li,
  • Yong Xiao,
  • Ming-Kai Chen,
  • Min Wu

DOI
https://doi.org/10.1186/s13059-023-03108-3
Journal volume & issue
Vol. 24, no. 1
pp. 1 – 23

Abstract

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Abstract Background Enhancer dysregulation is one of the important features for cancer cells. Enhancers enriched with H3K4me3 have been implicated to play important roles in cancer. However, their detailed features and regulatory mechanisms have not been well characterized. Results Here, we profile the landscape of H3K4me3-enriched enhancers (m3Es) in 43 pairs of colorectal cancer (CRC) samples. M3Es are widely distributed in CRC and averagely possess around 10% of total active enhancers. We identify 1322 gain variant m3Es and 367 lost variant m3Es in CRC. The target genes of the gain m3Es are enriched in immune response pathways. We experimentally prove that repression of CBX8 and RPS6KA5 m3Es inhibits target gene expression in CRC. Furthermore, we find histone methyltransferase MLL1 is responsible for depositing H3K4me3 on the identified Vm3Es. We demonstrate that the transcription factor AP1/JUN interacts with MLL1 and regulates m3E activity. Application of a small chemical inhibitor for MLL1 activity, OICR-9429, represses target gene expression of the identified Vm3Es, enhances anti-tumor immunity and inhibits CRC growth in an animal model. Conclusions Taken together, our study illustrates the genome-wide landscape and the regulatory mechanisms of m3Es in CRC, and reveals potential novel strategies for cancer treatment.

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