Cardiolipin coordinates inflammatory metabolic reprogramming through regulation of Complex II disassembly and degradation

心磷脂通过调节复合物 II 的分解和降解来协调炎症代谢重编程

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作者：Mack B Reynolds, Hanna S Hong, Britton C Michmerhuizen, Anna-Lisa E Lawrence, Li Zhang, Jason S Knight, Costas A Lyssiotis, Basel H Abuaita, Mary X O'Riordan

期刊：

Science Advances

影响因子：

11.700

时间：

2023

起止号：

2023 Feb 3;9(5):eade8701.

doi：

10.1126/sciadv.ade8701

研究方向：

代谢

Abstract

Macrophage metabolic plasticity enables repurposing of electron transport from energy generation to inflammation and host defense. Altered respiratory complex II function has been implicated in cancer, diabetes, and inflammation, but regulatory mechanisms are incompletely understood. Here, we show that macrophage inflammatory activation triggers Complex II disassembly and succinate dehydrogenase subunit B loss through sequestration and selective mitophagy. Mitochondrial fission supported lipopolysaccharide-stimulated succinate dehydrogenase subunit B degradation but not sequestration. We hypothesized that this Complex II regulatory mechanism might be coordinated by the mitochondrial phospholipid cardiolipin. Cardiolipin synthase knockdown prevented lipopolysaccharide-induced metabolic remodeling and Complex II disassembly, sequestration, and degradation. Cardiolipin-depleted macrophages were defective in lipopolysaccharide-induced pro-inflammatory cytokine production, a phenotype partially rescued by Complex II inhibition. Thus, cardiolipin acts as a critical organizer of inflammatory metabolic remodeling.

Cardiolipin coordinates inflammatory metabolic reprogramming through regulation of Complex II disassembly and degradation

心磷脂通过调节复合物 II 的分解和降解来协调炎症代谢重编程

Abstract

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