4.4 Article

Marham-Mafasel decrease joint inflammation and IL-1β gene expression in rheumatoid arthritis animal model

Journal

VETERINARY MEDICINE AND SCIENCE
Volume 7, Issue 4, Pages 1417-1425

Publisher

WILEY
DOI: 10.1002/vms3.430

Keywords

adjuvant; cytokine; herbal medicines; joint inflammation

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Marham-Mafasel can reduce joint inflammation, decrease IL-1 beta gene expression, and show significant therapeutic effects in animal experiments.
Background: Rheumatoid arthritis (RA) is a systemic chronic disease with synovial membrane, tendon and articular tissue inflammation. Current treatments of RA have many side effects and are quite expensive. Today, new treatments procedures and inexpensive herbal drugs are developed. Marham-Mafasel is mainly made out of two traditional herbs (Arnebia euchroma and Martricaria chamomilla). Objective: In this study, for the first time, the impact of Marham-Mafasel on joint inflammation, histopathological changes and IL-1 beta gene expression was evaluated in RA animal model. Methods: The RA was induced by a single s.c. injection of 0.1 ml Freund's complete adjuvant into the left hind footpad. In continuous, 15 RA male Wistar rats were used in three groups: I: Control; II: Treatment I (Piroxicam) and III: Treatment II (Marham-Mafasel). The volume of the hind paw was measured every day from 0 to 19 using water changed volume approach. The inflammation in the joint was evaluated using histopathology assay and gene expression of IL-1 beta was evaluated with use of Real-Time PCR. Results: Hind paw swelling of Marham-Mafasel at days 10th and 19th was reduced compared with the control group (p < 0.05). There was no statistically difference in histological degrading and changes index in three groups (p >= 0.05). Relative expression of IL-1 beta in Marham-Mafasel group was significantly decreased compared with other groups. Conclusion: The co-administration of M. Chamomile and A. euchroma, called Marham-Mafasel, decreases IL-1 beta gene expression that leads to a reduction in inflammation in rheumatoid arthritis (RA) animal model.

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