eLife (Jun 2018)

Chimeric antigen receptors that trigger phagocytosis

  • Meghan A Morrissey,
  • Adam P Williamson,
  • Adriana M Steinbach,
  • Edward W Roberts,
  • Nadja Kern,
  • Mark B Headley,
  • Ronald D Vale

DOI
https://doi.org/10.7554/eLife.36688
Journal volume & issue
Vol. 7

Abstract

Read online

Chimeric antigen receptors (CARs) are synthetic receptors that reprogram T cells to kill cancer. The success of CAR-T cell therapies highlights the promise of programmed immunity and suggests that applying CAR strategies to other immune cell lineages may be beneficial. Here, we engineered a family of Chimeric Antigen Receptors for Phagocytosis (CAR-Ps) that direct macrophages to engulf specific targets, including cancer cells. CAR-Ps consist of an extracellular antibody fragment, which can be modified to direct CAR-P activity towards specific antigens. By screening a panel of engulfment receptor intracellular domains, we found that the cytosolic domains from Megf10 and FcRɣ robustly triggered engulfment independently of their native extracellular domain. We show that CAR-Ps drive specific engulfment of antigen-coated synthetic particles and whole human cancer cells. Addition of a tandem PI3K recruitment domain increased cancer cell engulfment. Finally, we show that CAR-P expressing murine macrophages reduce cancer cell number in co-culture by over 40%.

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