Schizophyllan Polysaccharide from Schizophyllum commune demonstrates antinociceptive effect on preclinical models of acute pain

Schizophyllan Polysaccharide from Schizophyllum commune demonstrates antinociceptive effect on preclinical models of acute pain

Introduction: Twenty-five to 29% of the global population experiences pain that motivates seeking emergency services. Objective: To evaluate the effect of schizophyllan glucan polysaccharide (SPG), an isolated β-(1→3),(1→6) glucan polysaccharide of Schizophyllum commune, in acute pain and neuromusc...

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Main Authors: Katherine Plautz, Gabriela Borgmann, Alessandra Betina Gastaldi, Gustavo Schuetzler Gomes Fernandes, Eduardo Manoel Pereira, Samira Dal-Toé de Prá, Nicole Dalonso, Débora Delwing-Dal Magro, Daniela Delwing-de Lima
Format: Article
Language:English
Published: Faculdade de Medicina do ABC 2025-04-01
Series:ABCS Health Sciences
Subjects:
acute pain
fungal polysaccharides
Schizophyllum
models, animal
analgesia
anti-inflammatory agents
Online Access:https://www.portalnepas.org.br/abcshs/article/view/2718
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Summary:Introduction: Twenty-five to 29% of the global population experiences pain that motivates seeking emergency services. Objective: To evaluate the effect of schizophyllan glucan polysaccharide (SPG), an isolated β-(1→3),(1→6) glucan polysaccharide of Schizophyllum commune, in acute pain and neuromuscular performance on pre-clinical models. Methods: Male adult Swiss mice (20-30g, 60 days) were acclimated for a week in groups of 7 per cage before the experiment. SPG was administered, intraperitoneally, at doses of 0.1, 1.0, 3.0, 5.0, 10.0, 30.0, and 100.0 mg/Kg for the writhing test, and 1.0, 10.0, and 30.0 mg/Kg for the formalin and Rotarod tests, respectively. Statistical analysis was performed using one-way ANOVA, followed by the Duncan post hoc test, respectively, as appropriate (p<0.05). Results: Regarding the abdominal writhing test, SPG doses of 1.0, 5.0, 10.0, 30.0, and 100.0 mg/Kg promoted a significant reduction in writing of, respectively, 90.6%, 86.6%, 83.0%, 86.6%, and 76.2%. In the formalin test, the dose of SPG 30 mg/Kg reduced phase II nociception time by 78.0%. Relevant sedation was observed only to SPG 100 mg/Kg in the Rotarod test. Conclusion: SPG showed significant analgesic effects on acute inflammatory pain without causing concomitant central nervous system depression.
ISSN:2318-4965
2357-8114

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