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A genome-wide CRISPR screen identifies WDFY3 as a regulator of macrophage efferocytosis

Author

Listed:
  • Jianting Shi

    (Columbia University Irving Medical Center)

  • Xun Wu

    (Columbia University Irving Medical Center)

  • Ziyi Wang

    (Columbia University Irving Medical Center)

  • Fang Li

    (Columbia University Irving Medical Center)

  • Yujiao Meng

    (Columbia University Irving Medical Center
    Beijing University of Chinese Medicine)

  • Rebecca M. Moore

    (Columbia University Irving Medical Center)

  • Jian Cui

    (Columbia University Irving Medical Center)

  • Chenyi Xue

    (Columbia University Irving Medical Center)

  • Katherine R. Croce

    (Columbia University)

  • Arif Yurdagul

    (Louisiana State University Health Sciences Center at Shreveport)

  • John G. Doench

    (Broad Institute of MIT and Harvard)

  • Wei Li

    (Center for Genetic Medicine Research, Children’s National Hospital
    George Washington University)

  • Konstantinos S. Zarbalis

    (Department of Pathology and Laboratory Medicine
    Shriners Hospitals for Children Northern California
    UC Davis MIND Institute)

  • Ira Tabas

    (Columbia University
    Columbia University
    Columbia University)

  • Ai Yamamoto

    (Columbia University
    Columbia University)

  • Hanrui Zhang

    (Columbia University Irving Medical Center)

Abstract

Phagocytic clearance of dying cells, termed efferocytosis, is essential for maintaining tissue homeostasis, yet our understanding of efferocytosis regulation remains incomplete. Here we perform a FACS-based, genome-wide CRISPR knockout screen in primary mouse macrophages to search for novel regulators of efferocytosis. The results show that Wdfy3 knockout in macrophages specifically impairs uptake, but not binding, of apoptotic cells due to defective actin disassembly. Additionally, WDFY3 interacts with GABARAP, thus facilitating LC3 lipidation and subsequent lysosomal acidification to permit the degradation of apoptotic cell components. Mechanistically, while the C-terminus of WDFY3 is sufficient to rescue the impaired degradation induced by Wdfy3 knockout, full-length WDFY3 is required to reconstitute the uptake of apoptotic cells. Finally, WDFY3 is also required for efficient efferocytosis in vivo in mice and in vitro in primary human macrophages. This work thus expands our knowledge of the mechanisms of macrophage efferocytosis, as well as supports genome-wide CRISPR screen as a platform for interrogating complex functional phenotypes in primary macrophages.

Suggested Citation

  • Jianting Shi & Xun Wu & Ziyi Wang & Fang Li & Yujiao Meng & Rebecca M. Moore & Jian Cui & Chenyi Xue & Katherine R. Croce & Arif Yurdagul & John G. Doench & Wei Li & Konstantinos S. Zarbalis & Ira Tab, 2022. "A genome-wide CRISPR screen identifies WDFY3 as a regulator of macrophage efferocytosis," Nature Communications, Nature, vol. 13(1), pages 1-19, December.
    • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-35604-8
    DOI: 10.1038/s41467-022-35604-8
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    References listed on IDEAS

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