Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1

BACKGROUND: Chronic changes caused by a high‐fat diet (HFD) may be associated with weakened lung function in obese patients. However, few studies have focused on the role of senescent cells in HFD‐induced pulmonary fibrosis. This study aimed to determine whether (i) obesity causes the accumulation o...

Descripción completa

Detalles Bibliográficos
Autores principales: Gu, Xin, Meng, Haoyu, Peng, Chengyi, Lin, Shiyu, Li, Baihong, Zhao, Lin, Yang, Xue, Wang, Guangyan, Cai, Wenyuan, Zhou, Jiawen, Liu, Shuiyuan, Wu, Peng, Du, Yingqiang, Jin, Jianliang, Wang, Xiaoyan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10285269/
https://www.ncbi.nlm.nih.gov/pubmed/37345264
http://dx.doi.org/10.1002/ctm2.1308
_version_ 1785061575832371200
author Gu, Xin
Meng, Haoyu
Peng, Chengyi
Lin, Shiyu
Li, Baihong
Zhao, Lin
Yang, Xue
Wang, Guangyan
Cai, Wenyuan
Zhou, Jiawen
Liu, Shuiyuan
Wu, Peng
Du, Yingqiang
Jin, Jianliang
Wang, Xiaoyan
author_facet Gu, Xin
Meng, Haoyu
Peng, Chengyi
Lin, Shiyu
Li, Baihong
Zhao, Lin
Yang, Xue
Wang, Guangyan
Cai, Wenyuan
Zhou, Jiawen
Liu, Shuiyuan
Wu, Peng
Du, Yingqiang
Jin, Jianliang
Wang, Xiaoyan
author_sort Gu, Xin
collection PubMed
description BACKGROUND: Chronic changes caused by a high‐fat diet (HFD) may be associated with weakened lung function in obese patients. However, few studies have focused on the role of senescent cells in HFD‐induced pulmonary fibrosis. This study aimed to determine whether (i) obesity causes the accumulation of aging cells in the lungs, (ii) p16 accumulation in aging epithelial cells or fibroblasts exacerbates long‐term HFD‐induced senescence‐associated pulmonary fibrosis (SAPF) and (iii) p16 deletion or clearance of aging cells ameliorates HFD‐induced SAPF through inactivation of the inflammasome and metabolic remodelling. METHODS: Twelve‐month old male mice of p16(INK4a) (hereafter p16) knockout (p16(−−) ) and wild‐type (WT), ApoE knockout (ApoE(−−) ) and ApoE(−−)p16(−−) were fed a HFD to induce obesity, and the effects of treatment with the senolytic drug ABT263 or the SGK1 specific inhibitor EMD638683 on fibrosis, inflammaging, gene expression, integrin‐inflammasome signalling and metabolism were examined. A549 and IMR‐90 cells were transduced with p16‐overexpressing adenovirus, and treated with palmitic and oleic acids (P&O) to induce steatosis in vitro. RESULTS: We found that long‐term HFD promoted the expression of p16 and the increase of senescent cells in the lung. P16 knockout or ABT263 treatment alleviated pulmonary fibrosis, the increase of senescent cells and senescence‐associated secretory phenotype (SASP) in HFD‐fed mice, as well as in P&O‐treated A549 and IMR‐90 cells. RNA sequencing and bioinformatics analyses revealed that p16 knockout inhibited activation of the integrin‐inflammasome pathway and cellular glycolysis. Mass spectrometry, co‐immunoprecipitation and GST pull‐down assays demonstrated that p16 bound to the N‐terminal of SGK1, thereby interfering with the interaction between the E3 ubiquitin ligase NEDD4L and SGK1, and subsequently inhibiting K48‐polyubiquitin‐dependent degradation of SGK1 mediated by the NEDD4L–Ubch5 complex. EMD638683 was found to alleviate HFD‐induced pulmonary fibrosis and activation of the integrin‐inflammasome pathway. CONCLUSION: P16 accumulation promoted activation of integrin– inflammasome pathway and cell glycolysis by binding to the N– terminal of SGK1, intefering with the interaction between the E3 ubiquitin ligase NEDD4L and SGK1, thereby inhibiting K48– polyubiquitin– dependent degradation of SGK1 mediated by the NEDD4L–Ubch5 complex. ABT263 or EMD638683 could be used as potential drugs to treat pulmonary fibrosis in obese patients.
format Online
Article
Text
id pubmed-10285269
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-102852692023-06-23 Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1 Gu, Xin Meng, Haoyu Peng, Chengyi Lin, Shiyu Li, Baihong Zhao, Lin Yang, Xue Wang, Guangyan Cai, Wenyuan Zhou, Jiawen Liu, Shuiyuan Wu, Peng Du, Yingqiang Jin, Jianliang Wang, Xiaoyan Clin Transl Med Research Articles BACKGROUND: Chronic changes caused by a high‐fat diet (HFD) may be associated with weakened lung function in obese patients. However, few studies have focused on the role of senescent cells in HFD‐induced pulmonary fibrosis. This study aimed to determine whether (i) obesity causes the accumulation of aging cells in the lungs, (ii) p16 accumulation in aging epithelial cells or fibroblasts exacerbates long‐term HFD‐induced senescence‐associated pulmonary fibrosis (SAPF) and (iii) p16 deletion or clearance of aging cells ameliorates HFD‐induced SAPF through inactivation of the inflammasome and metabolic remodelling. METHODS: Twelve‐month old male mice of p16(INK4a) (hereafter p16) knockout (p16(−−) ) and wild‐type (WT), ApoE knockout (ApoE(−−) ) and ApoE(−−)p16(−−) were fed a HFD to induce obesity, and the effects of treatment with the senolytic drug ABT263 or the SGK1 specific inhibitor EMD638683 on fibrosis, inflammaging, gene expression, integrin‐inflammasome signalling and metabolism were examined. A549 and IMR‐90 cells were transduced with p16‐overexpressing adenovirus, and treated with palmitic and oleic acids (P&O) to induce steatosis in vitro. RESULTS: We found that long‐term HFD promoted the expression of p16 and the increase of senescent cells in the lung. P16 knockout or ABT263 treatment alleviated pulmonary fibrosis, the increase of senescent cells and senescence‐associated secretory phenotype (SASP) in HFD‐fed mice, as well as in P&O‐treated A549 and IMR‐90 cells. RNA sequencing and bioinformatics analyses revealed that p16 knockout inhibited activation of the integrin‐inflammasome pathway and cellular glycolysis. Mass spectrometry, co‐immunoprecipitation and GST pull‐down assays demonstrated that p16 bound to the N‐terminal of SGK1, thereby interfering with the interaction between the E3 ubiquitin ligase NEDD4L and SGK1, and subsequently inhibiting K48‐polyubiquitin‐dependent degradation of SGK1 mediated by the NEDD4L–Ubch5 complex. EMD638683 was found to alleviate HFD‐induced pulmonary fibrosis and activation of the integrin‐inflammasome pathway. CONCLUSION: P16 accumulation promoted activation of integrin– inflammasome pathway and cell glycolysis by binding to the N– terminal of SGK1, intefering with the interaction between the E3 ubiquitin ligase NEDD4L and SGK1, thereby inhibiting K48– polyubiquitin– dependent degradation of SGK1 mediated by the NEDD4L–Ubch5 complex. ABT263 or EMD638683 could be used as potential drugs to treat pulmonary fibrosis in obese patients. John Wiley and Sons Inc. 2023-06-21 /pmc/articles/PMC10285269/ /pubmed/37345264 http://dx.doi.org/10.1002/ctm2.1308 Text en © 2023 The Authors. Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Gu, Xin
Meng, Haoyu
Peng, Chengyi
Lin, Shiyu
Li, Baihong
Zhao, Lin
Yang, Xue
Wang, Guangyan
Cai, Wenyuan
Zhou, Jiawen
Liu, Shuiyuan
Wu, Peng
Du, Yingqiang
Jin, Jianliang
Wang, Xiaoyan
Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title_full Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title_fullStr Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title_full_unstemmed Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title_short Inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting NEDD4L‐mediated K48‐polyubiquitin‐dependent degradation of SGK1
title_sort inflammasome activation and metabolic remodelling in p16‐positive aging cells aggravates high‐fat diet‐induced lung fibrosis by inhibiting nedd4l‐mediated k48‐polyubiquitin‐dependent degradation of sgk1
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10285269/
https://www.ncbi.nlm.nih.gov/pubmed/37345264
http://dx.doi.org/10.1002/ctm2.1308
work_keys_str_mv AT guxin inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT menghaoyu inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT pengchengyi inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT linshiyu inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT libaihong inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT zhaolin inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT yangxue inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT wangguangyan inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT caiwenyuan inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT zhoujiawen inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT liushuiyuan inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT wupeng inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT duyingqiang inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT jinjianliang inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1
AT wangxiaoyan inflammasomeactivationandmetabolicremodellinginp16positiveagingcellsaggravateshighfatdietinducedlungfibrosisbyinhibitingnedd4lmediatedk48polyubiquitindependentdegradationofsgk1

Ejemplares similares