Cellular & Molecular Biology Letters (Jan 2021)

Iron overload adversely effects bone marrow haematogenesis via SIRT-SOD2-mROS in a process ameliorated by curcumin

  • Shujuan Zhou,
  • Lan Sun,
  • Shanhu Qian,
  • Yongyong Ma,
  • Ruye Ma,
  • Yuqing Dong,
  • Yifen Shi,
  • Songfu Jiang,
  • Haige Ye,
  • Zhijian Shen,
  • Shenghui Zhang,
  • Jianping Shen,
  • Kang Yu,
  • Siqian Wang

DOI
https://doi.org/10.1186/s11658-020-00244-7
Journal volume & issue
Vol. 26, no. 1
pp. 1 – 15

Abstract

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Abstract Background Iron overload, which is common in patients with haematological disorders, is known to have a suppressive effect on haematogenesis. However, the mechanism for this effect is still unclear. The antioxidant curcumin has been reported to protect against iron overload-induced bone marrow damage through an as-yet-unknown mechanism. Methods We established iron overload cell and mouse models. Mitochondrial reactive oxygen species (mROS) levels, autophagy levels and the SIRT3/SOD2 pathway were examined in the models and in the bone marrow of patients with iron overload. Results Iron overload was shown to depress haematogenesis and induce mitochondrion-derived superoxide anion-dependent autophagic cell death. Iron loading decreased SIRT3 protein expression, promoted an increase in SOD2, and led to the elevation of mROS. Overexpression of SIRT3 reversed these effects. Curcumin treatment ameliorated peripheral blood cells generation, enhanced SIRT3 activity, decreased SOD2 acetylation, inhibited mROS production, and suppressed iron loading-induced autophagy. Conclusions Our results suggest that curcumin exerts a protective effect on bone marrow by reducing mROS-stimulated autophagic cell death in a manner dependent on the SIRT3/SOD2 pathway.

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