Sestrin2 protects dendrite cells against ferroptosis induced by sepsis

Sestrin2 protects dendrite cells against ferroptosis induced by sepsis

Abstract Ferroptosis is a nonapoptotic form of programmed cell death triggered by the accumulation of reactive oxygen species (ROS) depended on iron overload. Although most investigations focus on the relationship between ferroptosis and cancer, neurodegenerative diseases, and ischemia/reperfusion i...

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Main Authors: Jing-yan Li, Chao Ren, Li-Xue Wang, Ren-qi Yao, Ning Dong, Yao Wu, Ying-ping Tian, Yong-ming Yao
Format: Article
Language:English
Published: Nature Publishing Group 2021-09-01
Series:Cell Death and Disease
Online Access:https://doi.org/10.1038/s41419-021-04122-8
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spelling doaj-be5a27e0b7bd4e1789f5a8f6d342ce0f2021-09-05T11:14:41ZengNature Publishing GroupCell Death and Disease2041-48892021-09-0112911310.1038/s41419-021-04122-8Sestrin2 protects dendrite cells against ferroptosis induced by sepsisJing-yan Li0Chao Ren1Li-Xue Wang2Ren-qi Yao3Ning Dong4Yao Wu5Ying-ping Tian6Yong-ming Yao7Department of Emergency, The Second Hospital of Hebei Medical UniversityTranslational Medicine Research Center, Medical Innovation Research Division and Fourth Medical Center of the Chinese PLA General HospitalTranslational Medicine Research Center, Medical Innovation Research Division and Fourth Medical Center of the Chinese PLA General HospitalTranslational Medicine Research Center, Medical Innovation Research Division and Fourth Medical Center of the Chinese PLA General HospitalTranslational Medicine Research Center, Medical Innovation Research Division and Fourth Medical Center of the Chinese PLA General HospitalTranslational Medicine Research Center, Medical Innovation Research Division and Fourth Medical Center of the Chinese PLA General HospitalDepartment of Emergency, The Second Hospital of Hebei Medical UniversityDepartment of Emergency, The Second Hospital of Hebei Medical UniversityAbstract Ferroptosis is a nonapoptotic form of programmed cell death triggered by the accumulation of reactive oxygen species (ROS) depended on iron overload. Although most investigations focus on the relationship between ferroptosis and cancer, neurodegenerative diseases, and ischemia/reperfusion injury, research on ferroptosis induced by immune-related inflammatory diseases, especially sepsis, is scarce. Sestrin2 (Sesn2), a highly evolutionary and stress-responsive protein, is critically involved in defense against oxidative stress challenges. Upregulated expression of Sesn2 has been observed in preliminary experiments to have an antioxidative function in the context of an inflammatory response. Nevertheless, the underlying function of Sesn2 in inflammation-mediated ferroptosis in the immune system remains uncertain. The current study aimed to demonstrate the protective effect of Sesn2 on ferroptosis and even correlations with ferroptosis and the functions of ferroptotic-dendritic cells (DCs) stimulated with lipopolysaccharide (LPS). The mechanism underlying DCs protection from LPS-induced ferroptosis by Sesn2 was further explored in this study. We found that the immune response of DCs assessed by co-stimulatory phenotypes was gradually enhanced at the peak time of 12 h upon 1 μg/ml LPS stimulation while ferroptosis in DCs treated with LPS at 24 h was significantly detected. LPS-induced ferroptosis showed a suppressive impact on DCs in phenotypic maturation, which was conversely relieved by the ferroptotic inhibitor. Compared with wild-type (WT) mice, DCs in genetic defective mice of Sesn2 (Sesn2−/−) exhibited exacerbated ferroptosis. Furthermore, the protective effect of Sesn2 on ferroptosis was noticed to be associated with the ATF4-CHOP-CHAC1 pathway, eventually exacerbating ferroptosis by degrading of glutathione. These results indicate that Sesn2 can suppress the ferroptosis of DCs in sepsis by downregulating the ATF4-CHOP-CHAC1 signaling pathway, and it might play an antioxidative role.https://doi.org/10.1038/s41419-021-04122-8
collection DOAJ
language English
format Article
sources DOAJ
author Jing-yan Li
Chao Ren
Li-Xue Wang
Ren-qi Yao
Ning Dong
Yao Wu
Ying-ping Tian
Yong-ming Yao
spellingShingle Jing-yan Li
Chao Ren
Li-Xue Wang
Ren-qi Yao
Ning Dong
Yao Wu
Ying-ping Tian
Yong-ming Yao
Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
Cell Death and Disease
author_facet Jing-yan Li
Chao Ren
Li-Xue Wang
Ren-qi Yao
Ning Dong
Yao Wu
Ying-ping Tian
Yong-ming Yao
author_sort Jing-yan Li
title Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
title_short Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
title_full Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
title_fullStr Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
title_full_unstemmed Sestrin2 protects dendrite cells against ferroptosis induced by sepsis
title_sort sestrin2 protects dendrite cells against ferroptosis induced by sepsis
publisher Nature Publishing Group
series Cell Death and Disease
issn 2041-4889
publishDate 2021-09-01
description Abstract Ferroptosis is a nonapoptotic form of programmed cell death triggered by the accumulation of reactive oxygen species (ROS) depended on iron overload. Although most investigations focus on the relationship between ferroptosis and cancer, neurodegenerative diseases, and ischemia/reperfusion injury, research on ferroptosis induced by immune-related inflammatory diseases, especially sepsis, is scarce. Sestrin2 (Sesn2), a highly evolutionary and stress-responsive protein, is critically involved in defense against oxidative stress challenges. Upregulated expression of Sesn2 has been observed in preliminary experiments to have an antioxidative function in the context of an inflammatory response. Nevertheless, the underlying function of Sesn2 in inflammation-mediated ferroptosis in the immune system remains uncertain. The current study aimed to demonstrate the protective effect of Sesn2 on ferroptosis and even correlations with ferroptosis and the functions of ferroptotic-dendritic cells (DCs) stimulated with lipopolysaccharide (LPS). The mechanism underlying DCs protection from LPS-induced ferroptosis by Sesn2 was further explored in this study. We found that the immune response of DCs assessed by co-stimulatory phenotypes was gradually enhanced at the peak time of 12 h upon 1 μg/ml LPS stimulation while ferroptosis in DCs treated with LPS at 24 h was significantly detected. LPS-induced ferroptosis showed a suppressive impact on DCs in phenotypic maturation, which was conversely relieved by the ferroptotic inhibitor. Compared with wild-type (WT) mice, DCs in genetic defective mice of Sesn2 (Sesn2−/−) exhibited exacerbated ferroptosis. Furthermore, the protective effect of Sesn2 on ferroptosis was noticed to be associated with the ATF4-CHOP-CHAC1 pathway, eventually exacerbating ferroptosis by degrading of glutathione. These results indicate that Sesn2 can suppress the ferroptosis of DCs in sepsis by downregulating the ATF4-CHOP-CHAC1 signaling pathway, and it might play an antioxidative role.
url https://doi.org/10.1038/s41419-021-04122-8
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