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Mitochondrial complex I activity in microglia sustains neuroinflammation.

Authors :: Peruzzotti-Jametti L
Willis CM
Krzak G
Hamel R
Pirvan L
Ionescu RB
Reisz JA
Prag HA
Garcia-Segura ME
Wu V
Xiang Y
Barlas B
Casey AM
van den Bosch AMR
Nicaise AM
Roth L
Bates GR
Huang H
Prasad P
Vincent AE
Frezza C
Viscomi C
Balmus G
Takats Z
Marioni JC
D'Alessandro A
Murphy MP
Mohorianu I
Pluchino S
Source :: Nature [Nature] 2024 Apr; Vol. 628 (8006), pp. 195-203. Date of Electronic Publication: 2024 Mar 13.
Publication Year :: 2024
Abstract: Sustained smouldering, or low-grade activation, of myeloid cells is a common hallmark of several chronic neurological diseases, including multiple sclerosis <superscript>1</superscript> . Distinct metabolic and mitochondrial features guide the activation and the diverse functional states of myeloid cells <superscript>2</superscript> . However, how these metabolic features act to perpetuate inflammation of the central nervous system is unclear. Here, using a multiomics approach, we identify a molecular signature that sustains the activation of microglia through mitochondrial complex I activity driving reverse electron transport and the production of reactive oxygen species. Mechanistically, blocking complex I in pro-inflammatory microglia protects the central nervous system against neurotoxic damage and improves functional outcomes in an animal disease model in vivo. Complex I activity in microglia is a potential therapeutic target to foster neuroprotection in chronic inflammatory disorders of the central nervous system <superscript>3</superscript> .<br /> (© 2024. The Author(s).)