Effects of Mimosa Caesalpiniifolia Pre-formulation on the Intestinal Barrier During Sodium Dextran Sulfate-induced Colitis in Wistar Rats

Overview

Journal Biomedica

Specialty General Medicine

Date 2023 Jul 11

PMID 37433169

Authors

Aline Garnevi-Favero

Karina Nascimento-da Silva

Willian Rodrigues-Ribeiro

Caroline Marcantonio-Ferreira

Patricia Sartorelli

Leonardo Cardili

Rita De Cassia-Sinigaglia

Joice Naiara Bertaglia-Pereira

Marcelo Aparecido-da Silva

Wagner Vilegas

Marcelo Jose Dias-Silva

Ana Paula Ribeiro-Paiotti

Affiliations

Soon will be listed here.

Abstract

Introduction: Anti-inflammatories, immunosuppressants, and immunobiological are commonly used in the treatment of inflammatory bowel disease. However, some patients do not present an adequate response or lose effective response during the treatment. A recent study found a potential anti-inflammatory effect of the hydroalcoholic extract of Mimosa caesalpiniifolia on trinitrobenzene sulfonic acid-induced colitis in Wistar rats.

Objective: To evaluate the effects of M. caesalpiniifolia pre-formulation on the intestinal barrier using dextran sulfate sodium-induced colitis model.

Materials And Methods: Leaf extracts were prepared in 70% ethanol and dried with a Buchi B19 Mini-spray dryer using 20% Aerosil® solution. Thirty-two male Wistar rats were randomized into four groups: basal control, untreated colitis, pre-formulation control (125 mg/kg/day), and colitis treated with pre-formulation (125 mg/kg/day). Clinical activity index was recorded daily and all rats were euthanized on the ninth day. Colon fragments were fixed and processed for histological and ultrastructural analyses. Stool samples were collected and processed for analysis of the short-chain fatty acid.

Results: Treatment with the pre-formulation decreased the clinical activity (bloody diarrhea), inflammatory infiltrate, and the ulcers. Pre-formulation did not repair the epithelial barrier and there were no significant differences in the goblet cells index. There was a significant difference in butyrate levels in the rats treated with the pre-formulation.

Conclusions: The pre-formulation minimized the clinical symptoms of colitis and intestinal inflammation, but did not minimize damage to the intestinal barrier.

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