Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis

OBJECTIVES: To define the host mechanisms contributing to the pathological interferon (IFN) type 1 signature in Juvenile dermatomyositis (JDM). METHODS: RNA-sequencing was performed on CD4(+), CD8(+), CD14(+) and CD19(+) cells sorted from pretreatment and on-treatment JDM (pretreatment n=10, on-trea...

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Autores principales: Wilkinson, Meredyth G Ll, Moulding, Dale, McDonnell, Thomas C R, Orford, Michael, Wincup, Chris, Ting, Joanna Y J, Otto, Georg W, Restuadi, Restuadi, Kelberman, Daniel, Papadopoulou, Charalampia, Castellano, Sergi, Eaton, Simon, Deakin, Claire T, Rosser, Elizabeth C, Wedderburn, Lucy R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2023
Materias:
Myositis
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10176342/
https://www.ncbi.nlm.nih.gov/pubmed/36564154
http://dx.doi.org/10.1136/ard-2022-223469
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author Wilkinson, Meredyth G Ll
Moulding, Dale
McDonnell, Thomas C R
Orford, Michael
Wincup, Chris
Ting, Joanna Y J
Otto, Georg W
Restuadi, Restuadi
Kelberman, Daniel
Papadopoulou, Charalampia
Castellano, Sergi
Eaton, Simon
Deakin, Claire T
Rosser, Elizabeth C
Wedderburn, Lucy R
author_facet Wilkinson, Meredyth G Ll
Moulding, Dale
McDonnell, Thomas C R
Orford, Michael
Wincup, Chris
Ting, Joanna Y J
Otto, Georg W
Restuadi, Restuadi
Kelberman, Daniel
Papadopoulou, Charalampia
Castellano, Sergi
Eaton, Simon
Deakin, Claire T
Rosser, Elizabeth C
Wedderburn, Lucy R
author_sort Wilkinson, Meredyth G Ll
collection PubMed
description OBJECTIVES: To define the host mechanisms contributing to the pathological interferon (IFN) type 1 signature in Juvenile dermatomyositis (JDM). METHODS: RNA-sequencing was performed on CD4(+), CD8(+), CD14(+) and CD19(+) cells sorted from pretreatment and on-treatment JDM (pretreatment n=10, on-treatment n=11) and age/sex-matched child healthy-control (CHC n=4) peripheral blood mononuclear cell (PBMC). Mitochondrial morphology and superoxide were assessed by fluorescence microscopy, cellular metabolism by (13)C glucose uptake assays, and oxidised mitochondrial DNA (oxmtDNA) content by dot-blot. Healthy-control PBMC and JDM pretreatment PBMC were cultured with IFN-α, oxmtDNA, cGAS-inhibitor, TLR-9 antagonist and/or n-acetyl cysteine (NAC). IFN-stimulated gene (ISGs) expression was measured by qPCR. Total numbers of patient and controls for functional experiments, JDM n=82, total CHC n=35. RESULTS: Dysregulated mitochondrial-associated gene expression correlated with increased ISG expression in JDM CD14+ monocytes. Altered mitochondrial-associated gene expression was paralleled by altered mitochondrial biology, including ‘megamitochondria’, cellular metabolism and a decrease in gene expression of superoxide dismutase (SOD)1. This was associated with enhanced production of oxidised mitochondrial (oxmt)DNA. OxmtDNA induced ISG expression in healthy PBMC, which was blocked by targeting oxidative stress and intracellular nucleic acid sensing pathways. Complementary experiments showed that, under in vitro experimental conditions, targeting these pathways via the antioxidant drug NAC, TLR9 antagonist and to a lesser extent cGAS-inhibitor, suppressed ISG expression in pretreatment JDM PBMC. CONCLUSIONS: These results describe a novel pathway where altered mitochondrial biology in JDM CD14+ monocytes lead to oxmtDNA production and stimulates ISG expression. Targeting this pathway has therapeutical potential in JDM and other IFN type 1-driven autoimmune diseases.
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spelling pubmed-101763422023-05-13 Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis Wilkinson, Meredyth G Ll Moulding, Dale McDonnell, Thomas C R Orford, Michael Wincup, Chris Ting, Joanna Y J Otto, Georg W Restuadi, Restuadi Kelberman, Daniel Papadopoulou, Charalampia Castellano, Sergi Eaton, Simon Deakin, Claire T Rosser, Elizabeth C Wedderburn, Lucy R Ann Rheum Dis Myositis OBJECTIVES: To define the host mechanisms contributing to the pathological interferon (IFN) type 1 signature in Juvenile dermatomyositis (JDM). METHODS: RNA-sequencing was performed on CD4(+), CD8(+), CD14(+) and CD19(+) cells sorted from pretreatment and on-treatment JDM (pretreatment n=10, on-treatment n=11) and age/sex-matched child healthy-control (CHC n=4) peripheral blood mononuclear cell (PBMC). Mitochondrial morphology and superoxide were assessed by fluorescence microscopy, cellular metabolism by (13)C glucose uptake assays, and oxidised mitochondrial DNA (oxmtDNA) content by dot-blot. Healthy-control PBMC and JDM pretreatment PBMC were cultured with IFN-α, oxmtDNA, cGAS-inhibitor, TLR-9 antagonist and/or n-acetyl cysteine (NAC). IFN-stimulated gene (ISGs) expression was measured by qPCR. Total numbers of patient and controls for functional experiments, JDM n=82, total CHC n=35. RESULTS: Dysregulated mitochondrial-associated gene expression correlated with increased ISG expression in JDM CD14+ monocytes. Altered mitochondrial-associated gene expression was paralleled by altered mitochondrial biology, including ‘megamitochondria’, cellular metabolism and a decrease in gene expression of superoxide dismutase (SOD)1. This was associated with enhanced production of oxidised mitochondrial (oxmt)DNA. OxmtDNA induced ISG expression in healthy PBMC, which was blocked by targeting oxidative stress and intracellular nucleic acid sensing pathways. Complementary experiments showed that, under in vitro experimental conditions, targeting these pathways via the antioxidant drug NAC, TLR9 antagonist and to a lesser extent cGAS-inhibitor, suppressed ISG expression in pretreatment JDM PBMC. CONCLUSIONS: These results describe a novel pathway where altered mitochondrial biology in JDM CD14+ monocytes lead to oxmtDNA production and stimulates ISG expression. Targeting this pathway has therapeutical potential in JDM and other IFN type 1-driven autoimmune diseases. BMJ Publishing Group 2023-05 2022-12-23 /pmc/articles/PMC10176342/ /pubmed/36564154 http://dx.doi.org/10.1136/ard-2022-223469 Text en © Author(s) (or their employer(s)) 2023. Re-use permitted under CC BY. Published by BMJ. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution 4.0 Unported (CC BY 4.0) license, which permits others to copy, redistribute, remix, transform and build upon this work for any purpose, provided the original work is properly cited, a link to the licence is given, and indication of whether changes were made. See: https://creativecommons.org/licenses/by/4.0/.
spellingShingle Myositis
Wilkinson, Meredyth G Ll
Moulding, Dale
McDonnell, Thomas C R
Orford, Michael
Wincup, Chris
Ting, Joanna Y J
Otto, Georg W
Restuadi, Restuadi
Kelberman, Daniel
Papadopoulou, Charalampia
Castellano, Sergi
Eaton, Simon
Deakin, Claire T
Rosser, Elizabeth C
Wedderburn, Lucy R
Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title_full Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title_fullStr Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title_full_unstemmed Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title_short Role of CD14+ monocyte-derived oxidised mitochondrial DNA in the inflammatory interferon type 1 signature in juvenile dermatomyositis
title_sort role of cd14+ monocyte-derived oxidised mitochondrial dna in the inflammatory interferon type 1 signature in juvenile dermatomyositis
topic Myositis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10176342/
https://www.ncbi.nlm.nih.gov/pubmed/36564154
http://dx.doi.org/10.1136/ard-2022-223469
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