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Abstract TP38: Harnessing the Gut-Brain Axis: The Therapeutic Potential of Akkermansia and Its Exosomes in Ischemic Stroke Recovery

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Introduction: The gut-brain axis is pivotal in recovery after stroke, with the gut microbiome playing a significant role in neurological outcomes. Akkermansia muciniphila (AKK), a beneficial gut bacterium, has shown promise in metabolic conditions. We hypothesize that AKK and its exosomes (AKK-Exo) can enhance stroke recovery by modulating gut-brain interactions. Methods: Human study: fecal samples from 88 ischemic stroke (IS) patients and 23 healthy elderly were analyzed using 16S rDNA sequencing. Animal study: 6-8 months old male mice subjected to photothrombotic middle cerebral artery occlusion were treated intragastrically with either AKK or AKK-Exo. Neurological recovery was evaluated over 2 weeks, accompanied by 16S rDNA sequencing and metabolomics analysis of fecal and plasma samples. The RT-PCR, Western blotting, and immunofluorescence were employed to assess inflammation, microglial activation, and white matter (WM) remodeling in the brain. Results: Human study demonstrated that IS disrupts gut microbiota, with an increase in pathogenic bacteria like Parabacteroides and a decrease in beneficial microbes like Lachnospira . Patients with higher levels of AKK exhibited better neurological outcomes. In the mouse model, both AKK and AKK-Exo treatments resulted in improvements in neurological function, also led to a restructuring of gut microecology, characterized by a reduction in pro-inflammatory bacteria and an increase in beneficial species. Moreover, the treatments were associated with a decrease in pro-inflammatory cytokine levels in both the brain and intestines. Metabolomics analysis revealed a notable reduction in trimethylamine N-oxide and an increase in beneficial metabolites such as sphingolipids and flavonoids. These metabolic changes were correlated with improved neurological outcomes. Molecular analyses further demonstrated that AKK and AKK-Exo treatments promoted the integrity of the gut barrier, reduced systemic inflammation, and induced an anti-inflammatory M2 microglial phenotype and facilitated WM remodeling in the brain. Conclusion: This study underscores the therapeutic potential of AKK and its exosomes in promoting recovery after IS, highlighting their role in gut-brain axis modulation. Our findings suggest that AKK and AKK-Exo could serve as promising therapeutic agents for improving stroke outcomes through microbiome-based interventions. Keywords: Gut-brain axis, microbiome, ischemic stroke, Akkermansia, neuroinflammation
Title: Abstract TP38: Harnessing the Gut-Brain Axis: The Therapeutic Potential of Akkermansia and Its Exosomes in Ischemic Stroke Recovery
Description:
Introduction: The gut-brain axis is pivotal in recovery after stroke, with the gut microbiome playing a significant role in neurological outcomes.
Akkermansia muciniphila (AKK), a beneficial gut bacterium, has shown promise in metabolic conditions.
We hypothesize that AKK and its exosomes (AKK-Exo) can enhance stroke recovery by modulating gut-brain interactions.
Methods: Human study: fecal samples from 88 ischemic stroke (IS) patients and 23 healthy elderly were analyzed using 16S rDNA sequencing.
Animal study: 6-8 months old male mice subjected to photothrombotic middle cerebral artery occlusion were treated intragastrically with either AKK or AKK-Exo.
Neurological recovery was evaluated over 2 weeks, accompanied by 16S rDNA sequencing and metabolomics analysis of fecal and plasma samples.
The RT-PCR, Western blotting, and immunofluorescence were employed to assess inflammation, microglial activation, and white matter (WM) remodeling in the brain.
Results: Human study demonstrated that IS disrupts gut microbiota, with an increase in pathogenic bacteria like Parabacteroides and a decrease in beneficial microbes like Lachnospira .
Patients with higher levels of AKK exhibited better neurological outcomes.
In the mouse model, both AKK and AKK-Exo treatments resulted in improvements in neurological function, also led to a restructuring of gut microecology, characterized by a reduction in pro-inflammatory bacteria and an increase in beneficial species.
Moreover, the treatments were associated with a decrease in pro-inflammatory cytokine levels in both the brain and intestines.
Metabolomics analysis revealed a notable reduction in trimethylamine N-oxide and an increase in beneficial metabolites such as sphingolipids and flavonoids.
These metabolic changes were correlated with improved neurological outcomes.
Molecular analyses further demonstrated that AKK and AKK-Exo treatments promoted the integrity of the gut barrier, reduced systemic inflammation, and induced an anti-inflammatory M2 microglial phenotype and facilitated WM remodeling in the brain.
Conclusion: This study underscores the therapeutic potential of AKK and its exosomes in promoting recovery after IS, highlighting their role in gut-brain axis modulation.
Our findings suggest that AKK and AKK-Exo could serve as promising therapeutic agents for improving stroke outcomes through microbiome-based interventions.
Keywords: Gut-brain axis, microbiome, ischemic stroke, Akkermansia, neuroinflammation.

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