Poster preview
ePoster
AKKERMANSIA-ASSOCIATED METABOLIC REMODELING LINKS GUT MICROBIOTA CHANGES TO NEUROBEHAVIORAL RECOVERY FOLLOWING INVASIVE LASER ACUPUNCTURE
Halin Jeonand 2 co-authors
Kyung Hee University
FENS Forum 2026 (2026)
Barcelona, Spain
Board PS02-07PM-453
Presentation
Date TBA
Board: PS02-07PM-453
Event Information
Poster Board
PS02-07PM-453
Poster
View posterAbstract
Parkinson’s disease (PD) is characterized by progressive neurodegeneration accompanied by neuroinflammation and gastrointestinal dysfunction, increasingly recognized to involve the gut–brain axis. Invasive laser acupuncture (ILA) has shown therapeutic potential in PD; however, the underlying microbiota- and metabolite-associated mechanisms remain unclear. Here, we investigated whether ILA improves neurobehavioral outcomes by remodeling gut microbiota and serum metabolomic profiles in a chronic MPTP-induced mouse model of PD.
ILA significantly ameliorated motor deficits and gastrointestinal dysmotility, while attenuating dopaminergic neuron loss and neuroinflammation in the substantia nigra and striatum. Gut histopathology and inflammatory signaling in the ileum were also markedly improved. Full-length 16S rRNA sequencing revealed that ILA selectively reshaped gut microbiota composition, with a prominent increase in Akkermansia muciniphila. Untargeted serum metabolomics further demonstrated that ILA induced a distinct metabolic profile, characterized by increased conjugated bile acids and acyl-carnitines, alongside reduced keto-type secondary bile acids.
To integrate microbiome, metabolome, and host phenotypes, we constructed an Akkermansia-aligned metabolic signature based on correlation-weighted metabolites. This composite signature showed strong associations with Akkermansia muciniphila abundance and neurobehavioral improvements, supporting a neurobehaviorally relevant gut–microbiota–metabolite axis. Triangulation analysis confirmed consistent relationships among Akkermansia abundance, the metabolic signature, and behavioral outcomes.
Collectively, these findings suggest that ILA promotes neurobehavioral recovery by remodeling gut microbiota and Akkermansia-associated metabolic pathways, highlighting a microbiota–metabolite–brain axis as a key mechanism underlying the therapeutic effects of ILA in Parkinsonian pathology.
ILA significantly ameliorated motor deficits and gastrointestinal dysmotility, while attenuating dopaminergic neuron loss and neuroinflammation in the substantia nigra and striatum. Gut histopathology and inflammatory signaling in the ileum were also markedly improved. Full-length 16S rRNA sequencing revealed that ILA selectively reshaped gut microbiota composition, with a prominent increase in Akkermansia muciniphila. Untargeted serum metabolomics further demonstrated that ILA induced a distinct metabolic profile, characterized by increased conjugated bile acids and acyl-carnitines, alongside reduced keto-type secondary bile acids.
To integrate microbiome, metabolome, and host phenotypes, we constructed an Akkermansia-aligned metabolic signature based on correlation-weighted metabolites. This composite signature showed strong associations with Akkermansia muciniphila abundance and neurobehavioral improvements, supporting a neurobehaviorally relevant gut–microbiota–metabolite axis. Triangulation analysis confirmed consistent relationships among Akkermansia abundance, the metabolic signature, and behavioral outcomes.
Collectively, these findings suggest that ILA promotes neurobehavioral recovery by remodeling gut microbiota and Akkermansia-associated metabolic pathways, highlighting a microbiota–metabolite–brain axis as a key mechanism underlying the therapeutic effects of ILA in Parkinsonian pathology.
Recommended posters
A COMPARATIVE STUDY ON THE EFFECTS OF "ANTI-PD GRANULES" AND PROBIOTICS ON THE INTESTINAL FLORA OF PARKINSON'S DISEASE MODEL MICE
Xiaohui Zhao, Juan Yang
EFFECT OF A PROBIOTIC TREATMENT ON AN EXTENDED EARLY-STAGE PARKINSON’S DISEASE MODEL
Saman Sabouni, Sara Fazzini, Andy Constanti, Emilio Russo, Audrey Mercer
A LIGHT-INDUCED PATHWAY THROUGH THE GUT-BRAIN AXIS FOR NEUROPROTECTION IN PARKINSON’S DISEASE
Yu Han Teng, He-Syun Chu, Shih-Kuo Chen
MAPPING OF VAGAL-DERIVED BRAINSTEM PATHWAYS AND THEIR POTENTIAL INFLUENCE IN DOPAMINERGIC NEURON DEGENERATION USING CONVENTIONAL AND MICROBIOTA-DEFICIENT MICE
Sena Güçer, Mélanie M. Depret, Linda Katona, John F. Cryan, Colin G. McNamara
ENVIRONMENTAL LIGHT MODULATION MITIGATES PARKINSON’S DISEASE PATHOLOGY
He Syun Chu, Ashley Hsieh, Yu-Han Teng, Shih-Kuo Chen
A COMMON INFLAMMATION-MIRNA AXIS DRIVES THE MOLECULAR CONVERGENCE OF PARKINSON'S DISEASE, DEPRESSIVE DISORDER, AND GUT DYSFUNCTION
Lluis Miquel-Rio, Judith Jericó-Escolar, Claudia Yanes-Castilla, Unai Sarriés-Serrano, Verónica Paz, Luis F Callado, J Javier Meana, Analia Bortolozzi