Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice

Background: Atherosclerosis (AS) is still the major cause of cardiovascular disease (CVD) as well as stroke. Endothelial metabolic disorder has been found to be activated and then promote endothelial cells (ECs) injury, which is regarded to initiate AS progression. N-acetylneuraminic acid (Neu5Ac),...

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Autores principales: Xiang, Peng, Chen, Qingqiu, Chen, Le, Lei, Jin, Yuan, Zhiyi, Hu, Hui, Lu, Yining, Wang, Xianmin, Wang, Tingting, Yu, Ruihong, Zhang, Wanping, Zhang, Jun, Yu, Chao, Ma, Limei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2023
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Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10526676/
https://www.ncbi.nlm.nih.gov/pubmed/37771765
http://dx.doi.org/10.7150/thno.87968
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author Xiang, Peng
Chen, Qingqiu
Chen, Le
Lei, Jin
Yuan, Zhiyi
Hu, Hui
Lu, Yining
Wang, Xianmin
Wang, Tingting
Yu, Ruihong
Zhang, Wanping
Zhang, Jun
Yu, Chao
Ma, Limei
author_facet Xiang, Peng
Chen, Qingqiu
Chen, Le
Lei, Jin
Yuan, Zhiyi
Hu, Hui
Lu, Yining
Wang, Xianmin
Wang, Tingting
Yu, Ruihong
Zhang, Wanping
Zhang, Jun
Yu, Chao
Ma, Limei
author_sort Xiang, Peng
collection PubMed
description Background: Atherosclerosis (AS) is still the major cause of cardiovascular disease (CVD) as well as stroke. Endothelial metabolic disorder has been found to be activated and then promote endothelial cells (ECs) injury, which is regarded to initiate AS progression. N-acetylneuraminic acid (Neu5Ac), a metabolite produced by hexosamine-sialic acid pathway branching from glucose metabolism, was presented as a notable biomarker of CVD and is positively correlated with ECs function. However, few studies explain whether Neu5Ac regulate AS progression by affecting EC function as well as its involved mechanisms are still unknown. Methods: Here, we mimicked an animal model in ApoE(-/-) mice which displaying similar plasma Neu5Ac levels with AS model to investigate its effect on AS progression. Results: We found that Neu5Ac exacerbated plaques area and increased lipids in plasma in absence of HFD feeding, and ECs inflammatory injury was supposed as the triggering factor upon Neu5Ac treatment with increasing expression of IL-1β, ICAM-1, and promoting ability of monocyte adhesion to ECs. Mechanistic studies showed that Neu5Ac facilitated SLC3A2 binding to ubiquitin and then triggered P62 mediated degradation, further leading to accumulation of lipid peroxidation in ECs. Fer-1 could inhibit ECs injury and reverse AS progression induced by Neu5Ac in ApoE(-/-) mice. Interestingly, mitochondrial dysfunction was also partly participated in ECs injury after Neu5Ac treatment and been reversed by Fer-1. Conclusions: Together, our study unveils a new mechanism by which evaluated metabolite Neu5Ac could promote SLC3A2 associated endothelial ferroptosis to activate ECs injury and AS plaque progression, thus providing a new insight into the role of Neu5Ac-ferroptosis pathway in AS. Also, our research revealed that pharmacological inhibition of ferroptosis may provide a novel therapeutic strategy for premature AS.
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spelling pubmed-105266762023-09-28 Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice Xiang, Peng Chen, Qingqiu Chen, Le Lei, Jin Yuan, Zhiyi Hu, Hui Lu, Yining Wang, Xianmin Wang, Tingting Yu, Ruihong Zhang, Wanping Zhang, Jun Yu, Chao Ma, Limei Theranostics Research Paper Background: Atherosclerosis (AS) is still the major cause of cardiovascular disease (CVD) as well as stroke. Endothelial metabolic disorder has been found to be activated and then promote endothelial cells (ECs) injury, which is regarded to initiate AS progression. N-acetylneuraminic acid (Neu5Ac), a metabolite produced by hexosamine-sialic acid pathway branching from glucose metabolism, was presented as a notable biomarker of CVD and is positively correlated with ECs function. However, few studies explain whether Neu5Ac regulate AS progression by affecting EC function as well as its involved mechanisms are still unknown. Methods: Here, we mimicked an animal model in ApoE(-/-) mice which displaying similar plasma Neu5Ac levels with AS model to investigate its effect on AS progression. Results: We found that Neu5Ac exacerbated plaques area and increased lipids in plasma in absence of HFD feeding, and ECs inflammatory injury was supposed as the triggering factor upon Neu5Ac treatment with increasing expression of IL-1β, ICAM-1, and promoting ability of monocyte adhesion to ECs. Mechanistic studies showed that Neu5Ac facilitated SLC3A2 binding to ubiquitin and then triggered P62 mediated degradation, further leading to accumulation of lipid peroxidation in ECs. Fer-1 could inhibit ECs injury and reverse AS progression induced by Neu5Ac in ApoE(-/-) mice. Interestingly, mitochondrial dysfunction was also partly participated in ECs injury after Neu5Ac treatment and been reversed by Fer-1. Conclusions: Together, our study unveils a new mechanism by which evaluated metabolite Neu5Ac could promote SLC3A2 associated endothelial ferroptosis to activate ECs injury and AS plaque progression, thus providing a new insight into the role of Neu5Ac-ferroptosis pathway in AS. Also, our research revealed that pharmacological inhibition of ferroptosis may provide a novel therapeutic strategy for premature AS. Ivyspring International Publisher 2023-09-04 /pmc/articles/PMC10526676/ /pubmed/37771765 http://dx.doi.org/10.7150/thno.87968 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Xiang, Peng
Chen, Qingqiu
Chen, Le
Lei, Jin
Yuan, Zhiyi
Hu, Hui
Lu, Yining
Wang, Xianmin
Wang, Tingting
Yu, Ruihong
Zhang, Wanping
Zhang, Jun
Yu, Chao
Ma, Limei
Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title_full Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title_fullStr Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title_full_unstemmed Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title_short Metabolite Neu5Ac triggers SLC3A2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in ApoE(-/-)mice
title_sort metabolite neu5ac triggers slc3a2 degradation promoting vascular endothelial ferroptosis and aggravates atherosclerosis progression in apoe(-/-)mice
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10526676/
https://www.ncbi.nlm.nih.gov/pubmed/37771765
http://dx.doi.org/10.7150/thno.87968
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