Scientific Reports (Jul 2017)

Interleukin 37 promotes angiogenesis through TGF-β signaling

  • Mengmeng Zhao,
  • Yongguang Hu,
  • Jiayi Jin,
  • Ying Yu,
  • Shanshan Zhang,
  • Jingjing Cao,
  • Yuanfen Zhai,
  • Rongbin Wei,
  • Juanjuan Shou,
  • Wenping Cai,
  • Shangfeng Liu,
  • Xiaoping Yang,
  • Guo-Tong Xu,
  • Jianhua Yang,
  • David B. Corry,
  • Shao Bo Su,
  • Xialin Liu,
  • Tianshu Yang

DOI
https://doi.org/10.1038/s41598-017-06124-z
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract IL-37 is a novel pro-angiogenic cytokine that potently promotes endothelial cell activation and pathological angiogenesis in our previous study, but the mechanisms behind the pro-angiogenic effect of IL-37 are less well understood. Extending our observations, we found that TGF-β interacts with IL-37, and potently enhances the binding affinity of IL-37 to the ALK1 receptor complex, thus allowing IL-37 to signal through ALK1 to activate pro-angiogenic responses. We further show that TGF-β and ALK1 are required in IL-37 induced pro-angiogenic response in ECs and in the mouse model of Matrigel plug and oxygen-induced retinopathy. The result suggests that IL-37 induces pro-angiogenic responses through TGF-β, which may act as the bridging molecule that mediates IL-37 binding to the TGF-β receptor complex.