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Bile acids target mitofusin 2 to differentially regulate innate immunity in physiological versus cholestatic conditions

Yuan Che, Wanfeng Xu, Chujie Ding, Tianyu He, Xiaowei Xu, Yubing Shuai, Hai Huang, Jiawei Wu, Yun Wang, Chen Wang, Guangji Wang, Lijuan Cao, Haiping Hao

2023Cell Reports59 citationsDOIOpen Access PDF

Abstract

Systemic metabolites serving as danger-associated molecular patterns play crucial roles in modulating the development, differentiation, and activity of innate immune cells. Yet, it is unclear how innate immune cells detect systemic metabolites for signal transmission. Here, we show that bile acids function as endogenous mitofusin 2 (MFN2) ligands and differentially modulate innate immune response to bacterial infection under cholestatic and physiological conditions. Bile acids at high concentrations promote mitochondrial tethering to the endoplasmic reticulum (ER), leading to calcium overload in the mitochondrion, which activates NLRP3 inflammasome and pyroptosis. By contrast, at physiologically relevant low concentrations, bile acids promote mitochondrial fusion, leading to enhanced oxidative phosphorylation and thereby strengthening infiltrated macrophages mediated phagocytotic clearance of bacteria. These findings support that bile acids, as endogenous activators of MFN2, are vital for tuning innate immune responses against infections, representing a causal link that connects systemic metabolism with mitochondrial dynamics in shaping innate immunity.

Topics & Concepts

Innate immune systemInflammasomeMFN2BiologyCell biologyImmune systemMitochondrionEndogenyEndoplasmic reticulumCD14Immunitymitochondrial fusionInflammationImmunologyBiochemistryMitochondrial DNAGeneInflammasome and immune disordersSphingolipid Metabolism and SignalingDrug Transport and Resistance Mechanisms
Bile acids target mitofusin 2 to differentially regulate innate immunity in physiological versus cholestatic conditions | Litcius