What does this research mean for the field?

Mitochondrial dysfunction during inflammatory stress reactivates ancient bacterial defense programs, contributing to diseases like sepsis and autoimmune disorders. Novelty: ClaimNovelty.SYNTHESIS. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

To examine the role of mitochondria in immunity and inflammation, highlighting the evolutionary transition from metabolic to immune functions.

March 6, 2026Open Access

From symbiosis to immunity: the evolutionary revival of mitochondrial defense programs in inflammatory diseases

Key Points

To examine the role of mitochondria in immunity and inflammation, highlighting the evolutionary transition from metabolic to immune functions.
Introduces Mitochondrial Endosymbiotic Dysregulation (MED) framework
Describes three stages of mitochondrial response to inflammatory stress
Analyzes structural and immunometabolic perspectives on mitochondrial remodeling
Mitochondrial dysfunction is reframed as an activation of ancient defense programs
Identifies three MED stages illustrating mitochondrial responses to stress
Discusses implications for diseases like sepsis and autoimmune disorders

Abstract

Mitochondria, descendants of ancestral α-proteobacteria, embody a dual identity that unites metabolic symbiosis with immune regulation. While evolution has transformed their form and function, mitochondria still preserve a tripartite heritage, an outer membrane resembling the host, an inner membrane of bacterial origin, and a matrix enriched with prokaryotic remnants such as unmethylated mitochondrial DNA (mtDNA), N-formyl peptides, and cardiolipin. Under physiological conditions, this architecture supports efficient energy generation while maintaining immunological silence. However, during infection, hypoxia, or systemic inflammation, this endosymbiotic equilibrium collapses, reawakening innate immune programs encoded in their bacterial ancestry. This review introduces the framework of Mitochondrial Endosymbiotic Dysregulation (MED) to describe the progressive transition of mitochondria from metabolic collaborators to immune activators under inflammatory stress. The MED model delineates three sequential stages: MED-I (Adaptive Remodeling), where mitochondria dynamically reorganize to preserve homeostasis, exhibiting characteristic structures such as mitochondrial flagella-like acquisition and retrieval extension (mitoFLARE) and mito-donut; MED-II (Functional Collapse), characterized by the failure of mitochondrial communication and the emergence of defensive structures such as mito-matryoshka; and MED-III (Structural Disintegration), marked by membrane rupture, release of mitochondrial damage-associated molecular patterns (DAMPs), and amplification of innate immune cascades. Rather than viewing mitochondrial dysfunction as a passive byproduct of injury, the MED paradigm reframes it as a reactivation of ancient bacterial defense programs, coupling bioenergetic failure to immune amplification. Thus, by integrating evolutionary, structural, and immunometabolic perspectives, this review discusses how mitochondrial remodeling under inflammatory stress contributes to diseases such as sepsis, autoimmune disorders, and neuroinflammation, and explores emerging therapeutic strategies aimed at restoring mitochondrial–host symbiosis.

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Cite This Study

Hong et al. (Wed,) studied this question.

synapsesocial.com/papers/69aa7008531e4c4a9ff59629 https://doi.org/https://doi.org/10.1186/s12964-026-02736-z

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