TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling

BACKGROUND & AIMS: Oxidative stress-mediated ferroptosis and macrophage-related inflammation play an important role in various liver diseases. Here, we explored if and how hepatocyte ferroptosis regulates macrophage stimulator of interferon genes (STING) activation in the development of spontane...

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Autores principales: Su, Wantong, Gao, Weicheng, Zhang, Rui, Wang, Qi, Li, Lei, Bu, Qingfa, Xu, Zibo, Liu, Zheng, Wang, Mingming, Zhu, Yaqing, Wu, Guoping, Zhou, Haoming, Wang, Xun, Lu, Ling
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10033999/
https://www.ncbi.nlm.nih.gov/pubmed/36968217
http://dx.doi.org/10.1016/j.jhepr.2023.100695
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author Su, Wantong
Gao, Weicheng
Zhang, Rui
Wang, Qi
Li, Lei
Bu, Qingfa
Xu, Zibo
Liu, Zheng
Wang, Mingming
Zhu, Yaqing
Wu, Guoping
Zhou, Haoming
Wang, Xun
Lu, Ling
author_facet Su, Wantong
Gao, Weicheng
Zhang, Rui
Wang, Qi
Li, Lei
Bu, Qingfa
Xu, Zibo
Liu, Zheng
Wang, Mingming
Zhu, Yaqing
Wu, Guoping
Zhou, Haoming
Wang, Xun
Lu, Ling
author_sort Su, Wantong
collection PubMed
description BACKGROUND & AIMS: Oxidative stress-mediated ferroptosis and macrophage-related inflammation play an important role in various liver diseases. Here, we explored if and how hepatocyte ferroptosis regulates macrophage stimulator of interferon genes (STING) activation in the development of spontaneous liver damage, fibrosis, and tumorigenesis. METHODS: We used a transforming growth factor-beta-activated kinase 1 (TAK1) deficiency-induced model of spontaneous liver damage, fibrosis, and tumorigenesis to investigate hepatocyte ferroptosis and its impact on macrophage STING signalling. Primary hepatocytes and macrophages were used for in vitro experiments. RESULTS: Significant liver injury and increased numbers of intrahepatic M1 macrophages were found in hepatocyte-specific TAK1-deficient (TAK1(ΔHEP)) mice, peaking at 4 weeks and gradually decreasing at 8 and 12 weeks. Meanwhile, activation of STING signalling was observed in livers from TAK1(ΔHEP) mice at 4 weeks and had decreased at 8 and 12 weeks. Treatment with a STING inhibitor promoted macrophage M2 polarisation and alleviated liver injury, fibrosis, and tumour burden. TAK1 deficiency exacerbated liver iron metabolism in mice with a high-iron diet. Moreover, consistent with the results from single-cell RNA-Seq dataset, TAK1(ΔHEP) mice demonstrated an increased oxidative response and hepatocellular ferroptosis, which could be inhibited by reactive oxygen species scavenging. Suppression of ferroptosis by ferrostatin-1 inhibited the activation of macrophage STING signalling, leading to attenuated liver injury and fibrosis and a reduced tumour burden. Mechanistically, increased intrahepatic and serum levels of 8-hydroxydeoxyguanosine were detected in TAK1(ΔHEP) mice, which was suppressed by ferroptosis inhibition. Treatment with 8-hydroxydeoxyguanosine antibody inhibited macrophage STING activation in TAK1(ΔHEP) mice. CONCLUSIONS: Hepatocellular ferroptosis-derived oxidative DNA damage promotes macrophage STING activation to facilitate the development of liver injury, fibrosis, and tumorigenesis. Inhibition of macrophage STING may represent a novel therapeutic approach for the prevention of chronic liver disease. IMPACT AND IMPLICATIONS: The precise mechanism by which hepatocyte ferroptosis regulates macrophage STING activation in the progression of liver damage, fibrosis, and tumorigenesis remains unclear. Herein, we show that deletion of TAK1 in hepatocytes caused oxidative stress-mediated ferroptosis and macrophage-related inflammation in the development of spontaneous liver injury, fibrosis, and hepatocellular carcinoma.
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spelling pubmed-100339992023-03-24 TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling Su, Wantong Gao, Weicheng Zhang, Rui Wang, Qi Li, Lei Bu, Qingfa Xu, Zibo Liu, Zheng Wang, Mingming Zhu, Yaqing Wu, Guoping Zhou, Haoming Wang, Xun Lu, Ling JHEP Rep Research Article BACKGROUND & AIMS: Oxidative stress-mediated ferroptosis and macrophage-related inflammation play an important role in various liver diseases. Here, we explored if and how hepatocyte ferroptosis regulates macrophage stimulator of interferon genes (STING) activation in the development of spontaneous liver damage, fibrosis, and tumorigenesis. METHODS: We used a transforming growth factor-beta-activated kinase 1 (TAK1) deficiency-induced model of spontaneous liver damage, fibrosis, and tumorigenesis to investigate hepatocyte ferroptosis and its impact on macrophage STING signalling. Primary hepatocytes and macrophages were used for in vitro experiments. RESULTS: Significant liver injury and increased numbers of intrahepatic M1 macrophages were found in hepatocyte-specific TAK1-deficient (TAK1(ΔHEP)) mice, peaking at 4 weeks and gradually decreasing at 8 and 12 weeks. Meanwhile, activation of STING signalling was observed in livers from TAK1(ΔHEP) mice at 4 weeks and had decreased at 8 and 12 weeks. Treatment with a STING inhibitor promoted macrophage M2 polarisation and alleviated liver injury, fibrosis, and tumour burden. TAK1 deficiency exacerbated liver iron metabolism in mice with a high-iron diet. Moreover, consistent with the results from single-cell RNA-Seq dataset, TAK1(ΔHEP) mice demonstrated an increased oxidative response and hepatocellular ferroptosis, which could be inhibited by reactive oxygen species scavenging. Suppression of ferroptosis by ferrostatin-1 inhibited the activation of macrophage STING signalling, leading to attenuated liver injury and fibrosis and a reduced tumour burden. Mechanistically, increased intrahepatic and serum levels of 8-hydroxydeoxyguanosine were detected in TAK1(ΔHEP) mice, which was suppressed by ferroptosis inhibition. Treatment with 8-hydroxydeoxyguanosine antibody inhibited macrophage STING activation in TAK1(ΔHEP) mice. CONCLUSIONS: Hepatocellular ferroptosis-derived oxidative DNA damage promotes macrophage STING activation to facilitate the development of liver injury, fibrosis, and tumorigenesis. Inhibition of macrophage STING may represent a novel therapeutic approach for the prevention of chronic liver disease. IMPACT AND IMPLICATIONS: The precise mechanism by which hepatocyte ferroptosis regulates macrophage STING activation in the progression of liver damage, fibrosis, and tumorigenesis remains unclear. Herein, we show that deletion of TAK1 in hepatocytes caused oxidative stress-mediated ferroptosis and macrophage-related inflammation in the development of spontaneous liver injury, fibrosis, and hepatocellular carcinoma. Elsevier 2023-02-03 /pmc/articles/PMC10033999/ /pubmed/36968217 http://dx.doi.org/10.1016/j.jhepr.2023.100695 Text en © 2023 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Article
Su, Wantong
Gao, Weicheng
Zhang, Rui
Wang, Qi
Li, Lei
Bu, Qingfa
Xu, Zibo
Liu, Zheng
Wang, Mingming
Zhu, Yaqing
Wu, Guoping
Zhou, Haoming
Wang, Xun
Lu, Ling
TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title_full TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title_fullStr TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title_full_unstemmed TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title_short TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling
title_sort tak1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cgas-sting signalling
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10033999/
https://www.ncbi.nlm.nih.gov/pubmed/36968217
http://dx.doi.org/10.1016/j.jhepr.2023.100695
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