Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver

BACKGROUND & AIMS: During liver fibrosis, tissue repair mechanisms replace necrotic tissue with highly stabilized extracellular matrix proteins. Extracellular matrix stabilization influences the speed of tissue recovery. Here, we studied the expression and function of peroxidasin (PXDN), a perox...

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Autores principales: Sojoodi, Mozhdeh, Erstad, Derek J., Barrett, Stephen C., Salloum, Shadi, Zhu, Shijia, Qian, Tongqi, Colon, Selene, Gale, Eric M., Jordan, Veronica Clavijo, Wang, Yongtao, Li, Shen, Ataeinia, Bahar, Jalilifiroozinezhad, Sasan, Lanuti, Michael, Zukerberg, Lawrence, Caravan, Peter, Hoshida, Yujin, Chung, Raymond T., Bhave, Gautam, Lauer, Georg M., Fuchs, Bryan C., Tanabe, Kenneth K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9043497/
https://www.ncbi.nlm.nih.gov/pubmed/35093588
http://dx.doi.org/10.1016/j.jcmgh.2022.01.015
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author Sojoodi, Mozhdeh
Erstad, Derek J.
Barrett, Stephen C.
Salloum, Shadi
Zhu, Shijia
Qian, Tongqi
Colon, Selene
Gale, Eric M.
Jordan, Veronica Clavijo
Wang, Yongtao
Li, Shen
Ataeinia, Bahar
Jalilifiroozinezhad, Sasan
Lanuti, Michael
Zukerberg, Lawrence
Caravan, Peter
Hoshida, Yujin
Chung, Raymond T.
Bhave, Gautam
Lauer, Georg M.
Fuchs, Bryan C.
Tanabe, Kenneth K.
author_facet Sojoodi, Mozhdeh
Erstad, Derek J.
Barrett, Stephen C.
Salloum, Shadi
Zhu, Shijia
Qian, Tongqi
Colon, Selene
Gale, Eric M.
Jordan, Veronica Clavijo
Wang, Yongtao
Li, Shen
Ataeinia, Bahar
Jalilifiroozinezhad, Sasan
Lanuti, Michael
Zukerberg, Lawrence
Caravan, Peter
Hoshida, Yujin
Chung, Raymond T.
Bhave, Gautam
Lauer, Georg M.
Fuchs, Bryan C.
Tanabe, Kenneth K.
author_sort Sojoodi, Mozhdeh
collection PubMed
description BACKGROUND & AIMS: During liver fibrosis, tissue repair mechanisms replace necrotic tissue with highly stabilized extracellular matrix proteins. Extracellular matrix stabilization influences the speed of tissue recovery. Here, we studied the expression and function of peroxidasin (PXDN), a peroxidase that uses hydrogen peroxide to cross-link collagen IV during liver fibrosis progression and regression. METHODS: Mouse models of liver fibrosis and cirrhosis patients were analyzed for the expression of PXDN in liver and serum. Pxdn(-/-) and Pxdn(+/+) mice were either treated with carbon tetrachloride for 6 weeks to generate toxin-induced fibrosis or fed with a choline-deficient L-amino acid-defined high-fat diet for 16 weeks to create nonalcoholic fatty liver disease fibrosis. Liver histology, quantitative real-time polymerase chain reaction, collagen content, flowcytometry and immunostaining of immune cells, RNA-sequencing, and liver function tests were analyzed. In vivo imaging of liver reactive oxygen species (ROS) was performed using a redox-active iron complex, Fe-PyC3A. RESULTS: In human and mouse cirrhotic tissue, PXDN is expressed by stellate cells and is secreted into fibrotic areas. In patients with nonalcoholic fatty liver disease, serum levels of PXDN increased significantly. In both mouse models of liver fibrosis, PXDN deficiency resulted in elevated monocyte and pro-fibrolysis macrophage recruitment into fibrotic bands and caused decreased accumulation of cross-linked collagens. In Pxdn(-/-) mice, collagen fibers were loosely organized, an atypical phenotype that is reversible upon macrophage depletion. Elevated ROS in Pxdn(-/-) livers was observed, which can result in activation of hypoxic signaling cascades and may affect signaling pathways involved in macrophage polarization such as TNF-a via NF-kB. Fibrosis resolution in Pxdn(-/-) mice was associated with significant decrease in collagen content and improved liver function. CONCLUSION: PXDN deficiency is associated with increased ROS levels and a hypoxic liver microenvironment that can regulate recruitment and programming of pro-resolution macrophages. Our data implicate the importance of the liver microenvironment in macrophage programming during liver fibrosis and suggest a novel pathway that is involved in the resolution of scar tissue.
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spelling pubmed-90434972022-04-28 Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver Sojoodi, Mozhdeh Erstad, Derek J. Barrett, Stephen C. Salloum, Shadi Zhu, Shijia Qian, Tongqi Colon, Selene Gale, Eric M. Jordan, Veronica Clavijo Wang, Yongtao Li, Shen Ataeinia, Bahar Jalilifiroozinezhad, Sasan Lanuti, Michael Zukerberg, Lawrence Caravan, Peter Hoshida, Yujin Chung, Raymond T. Bhave, Gautam Lauer, Georg M. Fuchs, Bryan C. Tanabe, Kenneth K. Cell Mol Gastroenterol Hepatol Original Research BACKGROUND & AIMS: During liver fibrosis, tissue repair mechanisms replace necrotic tissue with highly stabilized extracellular matrix proteins. Extracellular matrix stabilization influences the speed of tissue recovery. Here, we studied the expression and function of peroxidasin (PXDN), a peroxidase that uses hydrogen peroxide to cross-link collagen IV during liver fibrosis progression and regression. METHODS: Mouse models of liver fibrosis and cirrhosis patients were analyzed for the expression of PXDN in liver and serum. Pxdn(-/-) and Pxdn(+/+) mice were either treated with carbon tetrachloride for 6 weeks to generate toxin-induced fibrosis or fed with a choline-deficient L-amino acid-defined high-fat diet for 16 weeks to create nonalcoholic fatty liver disease fibrosis. Liver histology, quantitative real-time polymerase chain reaction, collagen content, flowcytometry and immunostaining of immune cells, RNA-sequencing, and liver function tests were analyzed. In vivo imaging of liver reactive oxygen species (ROS) was performed using a redox-active iron complex, Fe-PyC3A. RESULTS: In human and mouse cirrhotic tissue, PXDN is expressed by stellate cells and is secreted into fibrotic areas. In patients with nonalcoholic fatty liver disease, serum levels of PXDN increased significantly. In both mouse models of liver fibrosis, PXDN deficiency resulted in elevated monocyte and pro-fibrolysis macrophage recruitment into fibrotic bands and caused decreased accumulation of cross-linked collagens. In Pxdn(-/-) mice, collagen fibers were loosely organized, an atypical phenotype that is reversible upon macrophage depletion. Elevated ROS in Pxdn(-/-) livers was observed, which can result in activation of hypoxic signaling cascades and may affect signaling pathways involved in macrophage polarization such as TNF-a via NF-kB. Fibrosis resolution in Pxdn(-/-) mice was associated with significant decrease in collagen content and improved liver function. CONCLUSION: PXDN deficiency is associated with increased ROS levels and a hypoxic liver microenvironment that can regulate recruitment and programming of pro-resolution macrophages. Our data implicate the importance of the liver microenvironment in macrophage programming during liver fibrosis and suggest a novel pathway that is involved in the resolution of scar tissue. Elsevier 2022-01-28 /pmc/articles/PMC9043497/ /pubmed/35093588 http://dx.doi.org/10.1016/j.jcmgh.2022.01.015 Text en © 2022 The Authors 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 Original Research
Sojoodi, Mozhdeh
Erstad, Derek J.
Barrett, Stephen C.
Salloum, Shadi
Zhu, Shijia
Qian, Tongqi
Colon, Selene
Gale, Eric M.
Jordan, Veronica Clavijo
Wang, Yongtao
Li, Shen
Ataeinia, Bahar
Jalilifiroozinezhad, Sasan
Lanuti, Michael
Zukerberg, Lawrence
Caravan, Peter
Hoshida, Yujin
Chung, Raymond T.
Bhave, Gautam
Lauer, Georg M.
Fuchs, Bryan C.
Tanabe, Kenneth K.
Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title_full Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title_fullStr Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title_full_unstemmed Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title_short Peroxidasin Deficiency Re-programs Macrophages Toward Pro-fibrolysis Function and Promotes Collagen Resolution in Liver
title_sort peroxidasin deficiency re-programs macrophages toward pro-fibrolysis function and promotes collagen resolution in liver
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9043497/
https://www.ncbi.nlm.nih.gov/pubmed/35093588
http://dx.doi.org/10.1016/j.jcmgh.2022.01.015
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