1. Academic Validation
  2. Microglial FoxO3a deficiency ameliorates ferroptosis-induced brain injury of intracerebral haemorrhage via regulating autophagy and heme oxygenase-1

Microglial FoxO3a deficiency ameliorates ferroptosis-induced brain injury of intracerebral haemorrhage via regulating autophagy and heme oxygenase-1

  • J Cell Mol Med. 2023 Oct 27. doi: 10.1111/jcmm.18007.
Rikang Wang 1 Zhi Liang 2 Xiaoyan Xue 3 Hua Mei 4 Lianru Ji 2 Bocheng Wang 1 Wenjin Chen 1 Chao Gao 1 Shun Yuan 2 Tao Wu 1 Hui Qi 1 Suifa Hu 2 Li Yi 1 Yonggui Song 2 Rifang Liao 5 Baodong Chen 1
Affiliations

Affiliations

  • 1 Department of Neurosurgery, Peking University Shenzhen Hospital, Shenzhen, China.
  • 2 Jiangxi University of Chinese Medicine, Nanchang, China.
  • 3 Ganzhou People's Hospital, Ganzhou, China.
  • 4 Department of Pharmacy, Guangdong No.2 Provincial People's Hospital, Guangzhou, China.
  • 5 Department of Pharmacy, Sun Yat-sen Memorial Hospital, Sun Yat-sen University, Guangzhou, China.
Abstract

Microglial HO-1 regulates iron metabolism in the brain. Intracerebral haemorrhage (ICH) shares features of Ferroptosis and necroptosis; hemin is an oxidized product of haemoglobin from lysed red blood cells, leading to secondary injury. However, little is known about the underlying molecular mechanisms attributable to secondary injury by hemin or ICH. In this study, we first show that FoxO3a was highly co-located with neurons and microglia but not astrocytes area of ICH model mice. Hemin activated FoxO3a/ATG-mediated Autophagy and HO-1 signalling resulting in Ferroptosis in vitro and in a mice model of brain haemorrhage. Accordingly, Autophagy Inhibitor Baf-A1 or HO-1 inhibitor ZnPP protected against hemin-induced Ferroptosis. Hemin promoted Ferroptosis of neuronal cells via FoxO3a/ATG-mediated Autophagy and HO-1 signalling pathway. Knock-down of FoxO3a inhibited Autophagy and prevented hemin-induced Ferroptosis dependent of HO-1 signalling. We first showed that hemin stimulated microglial FoxO3a/HO-1 expression and enhanced the microglial polarisation towards the M1 phenotype, while knockdown of microglial FoxO3a inhibited pro-inflammatory cytokine production in microglia. Furthermore, the microglia activation in the striatum showed significant along with a high expression level of FoxO3a in the ICH mice. We found that conditional knockout of FoxO3a in microglia in mice alleviated neurological deficits and microglia activation as well as ferroptosis-induced striatum injury in the autologous blood-induced ICH model. We demonstrate, for the first time, that FoxO3a/ATG-mediated Autophagy and HO-1 play an important role in microglial activation and ferroptosis-induced striatum injury of ICH, identifying a new therapeutic avenue for the treatment of ICH.

Keywords

FoxO3a; HO-1; ferroptosis; intracerebral haemorrhage; microglia.

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