Journal of Translational Medicine (Jan 2022)

GM-CSF impairs erythropoiesis by disrupting erythroblastic island formation via macrophages

  • Weijie Cao,
  • Wenjuan Fan,
  • Fang Wang,
  • Yinyin Zhang,
  • Guanghua Wu,
  • Xiaojing Shi,
  • Jian xiang Shi,
  • Fengcai Gao,
  • Meimei Yan,
  • Rong Guo,
  • Yingmei Li,
  • Wei Li,
  • Chunyan Du,
  • Zhongxing Jiang

DOI
https://doi.org/10.1186/s12967-021-03214-5
Journal volume & issue
Vol. 20, no. 1
pp. 1 – 17

Abstract

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Abstract Anemia is a significant complication of chronic inflammation and may be related to dysregulated activities among erythroblastic island (EBI) macrophages. GM-CSF was reported to be upregulated and attracted as a therapeutic target in many inflammatory diseases. Among EBIs, we found that the GM-CSF receptor is preferentially and highly expressed among EBI macrophages but not among erythroblasts. GM-CSF treatment significantly decreases human EBI formation in vitro by decreasing the adhesion molecule expression of CD163. RNA-sequence analysis suggests that GM-CSF treatment impairs the supporting function of human EBI macrophages during erythropoiesis. GM-CSF treatment also polarizes human EBI macrophages from M2-like type to M1-like type. In addition, GM-CSF decreases mouse bone marrow (BM) erythroblasts as well as EBI macrophages, leading to a reduction in EBI numbers. In defining the molecular mechanism at work, we found that GM-CSF treatment significantly decreases the adhesion molecule expression of CD163 and Vcam1 in vivo. Importantly, GM-CSF treatment also decreases the phagocytosis rate of EBI macrophages in mouse BM as well as decreases the expression of the engulfment-related molecules Mertk, Axl, and Timd4. In addition, GM-CSF treatment polarizes mouse BM EBI macrophages from M2-like type to M1-like type. Thus, we document that GM-CSF impairs EBI formation in mice and humans. Our findings support that targeting GM-CSF or reprogramming EBI macrophages might be a novel strategy to treat anemia resulting from inflammatory diseases.

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