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Antibody targeting of E3 ubiquitin ligases for receptor degradation

Author

Listed:
  • Hadir Marei

    (Genentech)

  • Wen-Ting K. Tsai

    (Genentech)

  • Yee-Seir Kee

    (Genentech)

  • Karen Ruiz

    (Genentech)

  • Jieyan He

    (Genentech)

  • Chris Cox

    (Genentech Inc)

  • Tao Sun

    (Genentech)

  • Sai Penikalapati

    (Genentech)

  • Pankaj Dwivedi

    (Genentech)

  • Meena Choi

    (Genentech)

  • David Kan

    (Genentech)

  • Pablo Saenz-Lopez

    (Genentech)

  • Kristel Dorighi

    (Genentech)

  • Pamela Zhang

    (Genentech)

  • Yvonne T. Kschonsak

    (Genentech)

  • Noelyn Kljavin

    (Genentech)

  • Dhara Amin

    (Genentech)

  • Ingrid Kim

    (Genentech)

  • Andrew G. Mancini

    (Genentech)

  • Thao Nguyen

    (Genentech)

  • Chunling Wang

    (Genentech)

  • Eric Janezic

    (Genentech)

  • Alexander Doan

    (Genentech)

  • Elaine Mai

    (Genentech)

  • Hongkang Xi

    (Genentech)

  • Chen Gu

    (Genentech)

  • Melanie Heinlein

    (Genentech)

  • Brian Biehs

    (Genentech)

  • Jia Wu

    (Genentech)

  • Isabelle Lehoux

    (Genentech)

  • Seth Harris

    (Genentech)

  • Laetitia Comps-Agrar

    (Genentech)

  • Dhaya Seshasayee

    (Genentech)

  • Frederic J. de Sauvage

    (Genentech)

  • Matthew Grimmer

    (Genentech)

  • Jing Li

    (Genentech)

  • Nicholas J. Agard

    (Genentech)

  • Felipe de Sousa e Melo

    (Genentech)

Abstract

Most current therapies that target plasma membrane receptors function by antagonizing ligand binding or enzymatic activities. However, typical mammalian proteins comprise multiple domains that execute discrete but coordinated activities. Thus, inhibition of one domain often incompletely suppresses the function of a protein. Indeed, targeted protein degradation technologies, including proteolysis-targeting chimeras1 (PROTACs), have highlighted clinically important advantages of target degradation over inhibition2. However, the generation of heterobifunctional compounds binding to two targets with high affinity is complex, particularly when oral bioavailability is required3. Here we describe the development of proteolysis-targeting antibodies (PROTABs) that tether cell-surface E3 ubiquitin ligases to transmembrane proteins, resulting in target degradation both in vitro and in vivo. Focusing on zinc- and ring finger 3 (ZNRF3), a Wnt-responsive ligase, we show that this approach can enable colorectal cancer-specific degradation. Notably, by examining a matrix of additional cell-surface E3 ubiquitin ligases and transmembrane receptors, we demonstrate that this technology is amendable for ‘on-demand’ degradation. Furthermore, we offer insights on the ground rules governing target degradation by engineering optimized antibody formats. In summary, this work describes a strategy for the rapid development of potent, bioavailable and tissue-selective degraders of cell-surface proteins.

Suggested Citation

  • Hadir Marei & Wen-Ting K. Tsai & Yee-Seir Kee & Karen Ruiz & Jieyan He & Chris Cox & Tao Sun & Sai Penikalapati & Pankaj Dwivedi & Meena Choi & David Kan & Pablo Saenz-Lopez & Kristel Dorighi & Pamela, 2022. "Antibody targeting of E3 ubiquitin ligases for receptor degradation," Nature, Nature, vol. 610(7930), pages 182-189, October.
    • Handle: RePEc:nat:nature:v:610:y:2022:i:7930:d:10.1038_s41586-022-05235-6
    DOI: 10.1038/s41586-022-05235-6
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    Citations

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    Cited by:

    1. Shasha Yao & Yi Wang & Qian Tang & Yujie Yin & Yu Geng & Lei Xu & Shifu Liang & Jiajia Xiang & Jiaqi Fan & Jianbin Tang & Jian Liu & Shiqun Shao & Youqing Shen, 2024. "A plug-and-play monofunctional platform for targeted degradation of extracellular proteins and vesicles," Nature Communications, Nature, vol. 15(1), pages 1-14, December.
    2. Yuan Liu & Jingwen Yang & Tianlu Wang & Mei Luo & Yamei Chen & Chengxuan Chen & Ze’ev Ronai & Yubin Zhou & Eytan Ruppin & Leng Han, 2023. "Expanding PROTACtable genome universe of E3 ligases," Nature Communications, Nature, vol. 14(1), pages 1-17, December.

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