NEUROIMMUNE CROSSTALK AND PHARMACOLOGICAL MODULATION OF SEGMENT REGENERATION
HUN-REN Balaton Limnological Research Institute
Presentation
Date TBA
Event Information
Poster Board
PS02-07PM-048
Poster
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Using mass spectrometry and histochemistry, we detected GABA, Glut, DA, and 5-HT in coelomocytes of the earthworm model, Eisenia andrei. Transcriptomic analysis of coelomocytes revealed both evolutionarily conserved and lineage-specific features: transcripts encoding GAD, GABA-B receptor, 5-HT transporter, DA transporter, 5-HT receptors, and DA receptors were identified, whereas transcripts for TRH, TPH, AADC, GABA-A receptor, and GABA transporters were absent. The presence of GABAergic components suggests an ancient role for inhibitory signaling in immune regulation, while the lack of monoamine synthesis points to later evolutionary innovations in vertebrates. Quantitative mass spectrometry of coelomocytes collected at 0, 3, 7, and 14 days post-amputation revealed significant increases in Glut, 5-HT, and DA, accompanied by decreased GABA levels at days 3 and 7, implicating neurotransmitters in early regeneration. Pharmacological manipulation using different concentrations of haloperidol (D1/D2 antagonist), ondansetron (5-HT3 antagonist), GABA, and their mixtures significantly impaired segment regeneration and tissue organization.
Together, these findings demonstrate that coelomocyte-mediated neurotransmitter homeostasis is essential for proper regeneration and support the idea that neuroimmune communication is an evolutionarily conserved mechanism with relevance to regenerative medicine.
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