Mebendazole, an anti-helminth drug, suppresses inflammation, oxidative stress and injury in a mouse model of ulcerative colitis

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作者
Moein Eskandari
Fereshteh Asgharzadeh
Mohammad Mostafa Askarnia-faal
Hamideh Naimi
Amir Avan
Mitra Ahadi
Hassan Vossoughinia
Masoumeh Gharib
Atena Soleimani
Niloufar Naghibzadeh
Gordon Ferns
Mikhail Ryzhikov
Majid Khazaei
Seyed Mahdi Hassanian
机构
[1] Mashhad University of Medical Sciences,Department of Clinical Biochemistry, Faculty of Medicine
[2] Mashhad University of Medical Sciences,Department of Medical Physiology, Faculty of Medicine
[3] Mashhad University of Medical Sciences,Metabolic Syndrome Research Center
[4] Mashhad University of Medical Sciences,Department of Human Genetics, Faculty of Medicine
[5] Mashhad University of Medical Sciences,Department of Gastroenterology and Hepatology, Faculty of Medicine
[6] Mashhad University of Medical Sciences,Department of Pathology, Faculty of Medicine
[7] Brighton & Sussex Medical School,School of Medicine
[8] Division of Medical Education,undefined
[9] Saint Louis University,undefined
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Mebendazole (MBZ) is an efficacious anthelmintic with known anti-inflammatory and fibrinolytic properties. In this study, we aimed to explore the protective effects of this FDA-approved drug against DSS-induced colitis in a murine model either alone or in combination with Sulfasalazine (SSZ), a standard therapy for ulcerative colitis. We found that MBZ significantly improved colitis disease activity index as assessed by changes in body weight, degree of stool consistency, rectal bleeding, and prolapse. We also found that MBZ ameliorated the colon histopathological score by attenuating crypt loss, mucosal damage, and inflammation score in colitis tissues. Similarly, DSS-induced colon shortening, colon weight loss, and increase in spleen weight were all abrogated in the presence of MBZ. Moreover, MBZ decreased inflammation, possibly by reducing oxidative stress markers, suppressing inflammatory cell infiltration, and down-regulation of inflammatory genes in colon tissues. Furthermore, MBZ potently reduced fibrosis by decreasing collagen deposition and down-regulating pro-fibrotic genes including Col 1a1 and Col 1a2 in colitis tissue homogenates. In conclusion, our study showed that this broad-spectrum anthelminthic could be repurposed as a novel therapy for ulcerative colitis without any observed side effects, however, regarding the concerns about the potential toxicity of MBZ in UC patients, future experiments on MBZ therapy in other models of UC is needed to completely address the toxicity concerns.
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