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Enhancer release and retargeting activates disease-susceptibility genes

Author

Listed:
  • Soohwan Oh

    (University of California San Diego)

  • Jiaofang Shao

    (McGovern Medical School, University of Texas Health Science Center)

  • Joydeep Mitra

    (Albert Einstein College of Medicine)

  • Feng Xiong

    (McGovern Medical School, University of Texas Health Science Center)

  • Matteo D’Antonio

    (University of California San Diego)

  • Ruoyu Wang

    (McGovern Medical School, University of Texas Health Science Center
    University of Texas MD Anderson Cancer Center and UTHealth)

  • Ivan Garcia-Bassets

    (University of California San Diego)

  • Qi Ma

    (University of California San Diego)

  • Xiaoyu Zhu

    (McGovern Medical School, University of Texas Health Science Center)

  • Joo-Hyung Lee

    (McGovern Medical School, University of Texas Health Science Center)

  • Sreejith J. Nair

    (University of California San Diego)

  • Feng Yang

    (University of California San Diego)

  • Kenneth Ohgi

    (University of California San Diego)

  • Kelly A. Frazer

    (University of California San Diego
    University of California San Diego)

  • Zhengdong D. Zhang

    (Albert Einstein College of Medicine)

  • Wenbo Li

    (McGovern Medical School, University of Texas Health Science Center
    University of Texas MD Anderson Cancer Center and UTHealth)

  • Michael G. Rosenfeld

    (University of California San Diego)

Abstract

The functional engagement between an enhancer and its target promoter ensures precise gene transcription1. Understanding the basis of promoter choice by enhancers has important implications for health and disease. Here we report that functional loss of a preferred promoter can release its partner enhancer to loop to and activate an alternative promoter (or alternative promoters) in the neighbourhood. We refer to this target-switching process as ‘enhancer release and retargeting’. Genetic deletion, motif perturbation or mutation, and dCas9-mediated CTCF tethering reveal that promoter choice by an enhancer can be determined by the binding of CTCF at promoters, in a cohesin-dependent manner—consistent with a model of ‘enhancer scanning’ inside the contact domain. Promoter-associated CTCF shows a lower affinity than that at chromatin domain boundaries and often lacks a preferred motif orientation or a partnering CTCF at the cognate enhancer, suggesting properties distinct from boundary CTCF. Analyses of cancer mutations, data from the GTEx project and risk loci from genome-wide association studies, together with a focused CRISPR interference screen, reveal that enhancer release and retargeting represents an overlooked mechanism that underlies the activation of disease-susceptibility genes, as exemplified by a risk locus for Parkinson’s disease (NUCKS1–RAB7L1) and three loci associated with cancer (CLPTM1L–TERT, ZCCHC7–PAX5 and PVT1–MYC).

Suggested Citation

  • Soohwan Oh & Jiaofang Shao & Joydeep Mitra & Feng Xiong & Matteo D’Antonio & Ruoyu Wang & Ivan Garcia-Bassets & Qi Ma & Xiaoyu Zhu & Joo-Hyung Lee & Sreejith J. Nair & Feng Yang & Kenneth Ohgi & Kelly, 2021. "Enhancer release and retargeting activates disease-susceptibility genes," Nature, Nature, vol. 595(7869), pages 735-740, July.
    • Handle: RePEc:nat:nature:v:595:y:2021:i:7869:d:10.1038_s41586-021-03577-1
    DOI: 10.1038/s41586-021-03577-1
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    Citations

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    Cited by:

    1. Feng Bai & Peng Shu & Heng Deng & Yi Wu & Yao Chen & Mengbo Wu & Tao Ma & Yang Zhang & Julien Pirrello & Zhengguo Li & Yiguo Hong & Mondher Bouzayen & Mingchun Liu, 2024. "A distal enhancer guides the negative selection of toxic glycoalkaloids during tomato domestication," Nature Communications, Nature, vol. 15(1), pages 1-13, December.
    2. Sangram Kadam & Kiran Kumari & Vinoth Manivannan & Shuvadip Dutta & Mithun K. Mitra & Ranjith Padinhateeri, 2023. "Predicting scale-dependent chromatin polymer properties from systematic coarse-graining," Nature Communications, Nature, vol. 14(1), pages 1-14, December.
    3. Irene Robles-Rebollo & Sergi Cuartero & Adria Canellas-Socias & Sarah Wells & Mohammad M. Karimi & Elisabetta Mereu & Alexandra G. Chivu & Holger Heyn & Chad Whilding & Dirk Dormann & Samuel Marguerat, 2022. "Cohesin couples transcriptional bursting probabilities of inducible enhancers and promoters," Nature Communications, Nature, vol. 13(1), pages 1-16, December.
    4. Matteo D’Antonio & Jennifer P. Nguyen & Timothy D. Arthur & Hiroko Matsui & Agnieszka D’Antonio-Chronowska & Kelly A. Frazer, 2023. "Fine mapping spatiotemporal mechanisms of genetic variants underlying cardiac traits and disease," Nature Communications, Nature, vol. 14(1), pages 1-18, December.
    5. Mingsen Li & Huaxing Huang & Bofeng Wang & Shaoshuai Jiang & Huizhen Guo & Liqiong Zhu & Siqi Wu & Jiafeng Liu & Li Wang & Xihong Lan & Wang Zhang & Jin Zhu & Fuxi Li & Jieying Tan & Zhen Mao & Chunqi, 2022. "Comprehensive 3D epigenomic maps define limbal stem/progenitor cell function and identity," Nature Communications, Nature, vol. 13(1), pages 1-16, December.
    6. Shuai Liu & Yaqiang Cao & Kairong Cui & Qingsong Tang & Keji Zhao, 2022. "Hi-TrAC reveals division of labor of transcription factors in organizing chromatin loops," Nature Communications, Nature, vol. 13(1), pages 1-17, December.

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