Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice

Mitochondrial dysfunction is a key driver of inflammatory responses in human disease. However, it remains unclear whether alterations in mitochondria-innate immune cross-talk contribute to the pathobiology of mitochondrial disorders and aging. Using the polymerase gamma (POLG) mutator model of mitoc...

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Autores principales: Lei, Yuanjiu, Guerra Martinez, Camila, Torres-Odio, Sylvia, Bell, Samantha L., Birdwell, Christine E., Bryant, Joshua D., Tong, Carl W., Watson, Robert O., West, Laura Ciaccia, West, A. Phillip
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for the Advancement of Science 2021
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8153723/
https://www.ncbi.nlm.nih.gov/pubmed/34039599
http://dx.doi.org/10.1126/sciadv.abe7548
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author Lei, Yuanjiu
Guerra Martinez, Camila
Torres-Odio, Sylvia
Bell, Samantha L.
Birdwell, Christine E.
Bryant, Joshua D.
Tong, Carl W.
Watson, Robert O.
West, Laura Ciaccia
West, A. Phillip
author_facet Lei, Yuanjiu
Guerra Martinez, Camila
Torres-Odio, Sylvia
Bell, Samantha L.
Birdwell, Christine E.
Bryant, Joshua D.
Tong, Carl W.
Watson, Robert O.
West, Laura Ciaccia
West, A. Phillip
author_sort Lei, Yuanjiu
collection PubMed
description Mitochondrial dysfunction is a key driver of inflammatory responses in human disease. However, it remains unclear whether alterations in mitochondria-innate immune cross-talk contribute to the pathobiology of mitochondrial disorders and aging. Using the polymerase gamma (POLG) mutator model of mitochondrial DNA instability, we report that aberrant activation of the type I interferon (IFN-I) innate immune axis potentiates immunometabolic dysfunction, reduces health span, and accelerates aging in mutator mice. Mechanistically, elevated IFN-I signaling suppresses activation of nuclear factor erythroid 2–related factor 2 (NRF2), which increases oxidative stress, enhances proinflammatory cytokine responses, and accelerates metabolic dysfunction. Ablation of IFN-I signaling attenuates hyperinflammatory phenotypes by restoring NRF2 activity and reducing aerobic glycolysis, which combine to lessen cardiovascular and myeloid dysfunction in aged mutator mice. These findings further advance our knowledge of how mitochondrial dysfunction shapes innate immune responses and provide a framework for understanding mitochondria-driven immunopathology in POLG-related disorders and aging.
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spelling pubmed-81537232021-06-07 Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice Lei, Yuanjiu Guerra Martinez, Camila Torres-Odio, Sylvia Bell, Samantha L. Birdwell, Christine E. Bryant, Joshua D. Tong, Carl W. Watson, Robert O. West, Laura Ciaccia West, A. Phillip Sci Adv Research Articles Mitochondrial dysfunction is a key driver of inflammatory responses in human disease. However, it remains unclear whether alterations in mitochondria-innate immune cross-talk contribute to the pathobiology of mitochondrial disorders and aging. Using the polymerase gamma (POLG) mutator model of mitochondrial DNA instability, we report that aberrant activation of the type I interferon (IFN-I) innate immune axis potentiates immunometabolic dysfunction, reduces health span, and accelerates aging in mutator mice. Mechanistically, elevated IFN-I signaling suppresses activation of nuclear factor erythroid 2–related factor 2 (NRF2), which increases oxidative stress, enhances proinflammatory cytokine responses, and accelerates metabolic dysfunction. Ablation of IFN-I signaling attenuates hyperinflammatory phenotypes by restoring NRF2 activity and reducing aerobic glycolysis, which combine to lessen cardiovascular and myeloid dysfunction in aged mutator mice. These findings further advance our knowledge of how mitochondrial dysfunction shapes innate immune responses and provide a framework for understanding mitochondria-driven immunopathology in POLG-related disorders and aging. American Association for the Advancement of Science 2021-05-26 /pmc/articles/PMC8153723/ /pubmed/34039599 http://dx.doi.org/10.1126/sciadv.abe7548 Text en Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution NonCommercial License 4.0 (CC BY-NC). https://creativecommons.org/licenses/by-nc/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution-NonCommercial license (https://creativecommons.org/licenses/by-nc/4.0/) , which permits use, distribution, and reproduction in any medium, so long as the resultant use is not for commercial advantage and provided the original work is properly cited.
spellingShingle Research Articles
Lei, Yuanjiu
Guerra Martinez, Camila
Torres-Odio, Sylvia
Bell, Samantha L.
Birdwell, Christine E.
Bryant, Joshua D.
Tong, Carl W.
Watson, Robert O.
West, Laura Ciaccia
West, A. Phillip
Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title_full Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title_fullStr Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title_full_unstemmed Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title_short Elevated type I interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtDNA mutator mice
title_sort elevated type i interferon responses potentiate metabolic dysfunction, inflammation, and accelerated aging in mtdna mutator mice
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8153723/
https://www.ncbi.nlm.nih.gov/pubmed/34039599
http://dx.doi.org/10.1126/sciadv.abe7548
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