Cancer Medicine (Aug 2019)

Engineering macrophages to phagocytose cancer cells by blocking the CD47/SIRPɑ axis

  • Hongcheng Yang,
  • Ruoyang Shao,
  • Hongxin Huang,
  • Xinlong Wang,
  • Zhili Rong,
  • Ying Lin

DOI
https://doi.org/10.1002/cam4.2332
Journal volume & issue
Vol. 8, no. 9
pp. 4245 – 4253

Abstract

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Abstract The use of immunotherapy has achieved great advances in the treatment of cancer. Macrophages play a pivotal role in the immune defense system, serving both as phagocytes (removal of pathogens and cancer cells) and as antigen‐presenting cells (activation of T cells). However, research regarding tumor immunotherapy is mainly focused on the adaptive immune system. The usefulness of innate immune cells (eg, macrophages) in the treatment of cancer has not been extensively investigated. Recent advances in synthetic biology and the increasing understanding of the cluster of differentiation 47/signal regulatory protein alpha (CD47/SIRPɑ) axis may provide new opportunities for the clinical application of engineered macrophages. The CD47/SIRPɑ axis is a major known pathway, repressing phagocytosis and activation of macrophages. In this article, we summarize the currently available evidence regarding the CD47/SIRPɑ axis, and immunotherapies based on blockage. In addition, we propose cell therapy strategies based on macrophage engineering.

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