Journal
AGING CELL
Volume 21, Issue 6, Pages -Publisher
WILEY
DOI: 10.1111/acel.13622
Keywords
aging; macrophage; mitochondrial DNA; mitophagy; sterile inflammation; stimulator of interferon genes
Categories
Funding
- Major Program of the National Natural Science Foundation of China [81530048, 31930020]
- National Science and Technology Major Project [2018AD18]
- Key Laboratory of Liver Transplantation, Chinese Academy of Medical Sciences [2019PT320015]
- National Natural Science Foundation of China [82071798, 81870448, 81470901, 81901628]
- CAMS Innovation Fund for Medical Sciences [2019-I2 M-5-035]
- Jiangsu Provincial Natural Science Foundation [BK20191490]
- Six Talent Peaks Project in Jiangsu Province [2018-WSN-011]
- Jiangsu Science and Technology Association Young Science and Technology Talents Lifting Project [DG000D4007]
- Postgraduate Research & Practice Innovation Program of Jiangsu Province [KYCX21_1606]
- PAPD
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Aging impairs mitophagy and lysosomal function in macrophages, leading to the cytosolic release of mtDNA and increased STING activation. This promotes sterile inflammatory liver injury in aged patients. The findings suggest potential therapeutic targets for treating aged patients with sterile inflammatory liver injury.
Macrophage-stimulator of interferon genes (STING) signaling mediated sterile inflammation has been implicated in various age-related diseases. However, whether and how macrophage mitochondrial DNA (mtDNA) regulates STING signaling in aged macrophages remains largely unknown. We found that hypoxia-reoxygenation (HR) induced STING activation in macrophages by triggering the release of macrophage mtDNA into the cytosol. Aging promoted the cytosolic leakage of macrophage mtDNA and enhanced STING activation, which was abrogated upon mtDNA depletion or cyclic GMP-AMP Synthase (cGAS) inhibition. Aged macrophages exhibited increased mitochondrial injury with impaired mitophagy. Mechanistically, a decline in the PTEN-induced kinase 1 (PINK1)/Parkin-mediated polyubiquitination of mitochondria was observed in aged macrophages. Pink1 overexpression reversed the inhibition of mitochondrial ubiquitination but failed to promote mitolysosome formation in the aged macrophages. Meanwhile, aging impaired lysosomal biogenesis and function in macrophages by modulating the mTOR/transcription factor EB (TFEB) signaling pathway, which could be reversed by Torin-1 treatment. Consequently, Pink1 overexpression in combination with Torin-1 treatment restored mitophagic flux and inhibited mtDNA/cGAS/STING activation in aged macrophages. Moreover, besides HR-induced metabolic stress, other types of oxidative and hepatotoxic stresses inhibited mitophagy and promoted the cytosolic release of mtDNA to activate STING signaling in aged macrophages. STING deficiency protected aged mice against diverse types of sterile inflammatory liver injuries. Our findings suggest that aging impairs mitophagic flux to facilitate the leakage of macrophage mtDNA into the cytosol and promotes STING activation, and thereby provides a novel potential therapeutic target for sterile inflammatory liver injury in aged patients.
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