(-)-Fenchone Prevents Cysteamine-Induced Duodenal Ulcers and Accelerates Healing Promoting Re-Epithelialization of Gastric Ulcers in Rats via Antioxidant and Immunomodulatory Mechanisms

Maria Elaine Cristina Araruna; Edvaldo Balbino Alves Júnior; Catarina Alves de Lima Serafim; Matheus Marley Bezerra Pessoa; Michelle Liz de Souza Pessôa; Vitória Pereira Alves; Marcelo Sobral da Silva; Marianna Vieira Sobral; Adriano Francisco Alves; Mayara Karla dos Santos Nunes; Aurigena Antunes Araújo; Leônia Maria Batista

doi:10.3390/ph17050641

Pharmaceuticals (May 2024)

(-)-Fenchone Prevents Cysteamine-Induced Duodenal Ulcers and Accelerates Healing Promoting Re-Epithelialization of Gastric Ulcers in Rats via Antioxidant and Immunomodulatory Mechanisms

Maria Elaine Cristina Araruna,
Edvaldo Balbino Alves Júnior,
Catarina Alves de Lima Serafim,
Matheus Marley Bezerra Pessoa,
Michelle Liz de Souza Pessôa,
Vitória Pereira Alves,
Marcelo Sobral da Silva,
Marianna Vieira Sobral,
Adriano Francisco Alves,
Mayara Karla dos Santos Nunes,
Aurigena Antunes Araújo,
Leônia Maria Batista

Affiliations

Maria Elaine Cristina Araruna: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Edvaldo Balbino Alves Júnior: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Catarina Alves de Lima Serafim: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Matheus Marley Bezerra Pessoa: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Michelle Liz de Souza Pessôa: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Vitória Pereira Alves: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Marcelo Sobral da Silva: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Marianna Vieira Sobral: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Adriano Francisco Alves: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Mayara Karla dos Santos Nunes: Department of Physiology and Pathology, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil
Aurigena Antunes Araújo: Department of Morphology, Histology and Basic Pathology, Biosciences Center, Federal University of Rio Grande do Norte, Natal 59078-970, RN, Brazil
Leônia Maria Batista: Postgraduate Program in Natural and Synthetic Bioactive Products, Health Sciences Center, Federal University of Paraiba (UFPB), João Pessoa 58050-585, PB, Brazil

DOI: https://doi.org/10.3390/ph17050641
Journal volume & issue: Vol. 17, no. 5
p. 641

Abstract

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Background: (-)-Fenchone is a naturally occurring monoterpene found in the essential oils of Foeniculum vulgare Mill., Thuja occidentalis L., and Peumus boldus Molina. Pharmacological studies have reported its antinociceptive, antimicrobial, anti-inflammatory, antidiarrheal, and antioxidant activities. Methods: The preventive antiulcer effects of (-)-Fenchone were assessed through oral pretreatment in cysteamine-induced duodenal lesion models. Gastric healing, the underlying mechanisms, and toxicity after repeated doses were evaluated using the acetic acid-induced gastric ulcer rat model with oral treatment administered for 14 days. Results: In the cysteamine-induced duodenal ulcer model, fenchone (37.5–300 mg/kg) significantly decreased the ulcer area and prevented lesion formation. In the acetic acid-induced ulcer model, fenchone (150 mg/kg) reduced (p p < 0.001) malondialdehyde (MDA), myeloperoxidase (MPO), interleukin-1 beta (IL-1β), tumor necrosis factor-alpha (TNF-α), and nuclear transcription factor kappa B (NF-κB). A 14-day oral toxicity investigation revealed no alterations in heart, liver, spleen, or kidney weight, nor in the biochemical and hematological parameters assessed. (-)-Fenchone protected animals from body weight loss while maintaining feed and water intake. Conclusion: (-)-Fenchone exhibits low toxicity, prevents duodenal ulcers, and enhances gastric healing activities. Antioxidant and immunomodulatory properties appear to be involved in its therapeutic effects.

Published in Pharmaceuticals

ISSN: 1424-8247 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceuticals/

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