Sorafenib Reveals Anti-Arthritic Potentials in Collagen induced Experimental Arthritis Model
Date
2018Author
Gozel, Nevzat and Cakirer, Masallah and Karatas, Ahmet and Tuzcu, Mehmet
and Ozdemir, Fethi Ahmet and Dagli, Adile Ferda and Sahin, Kazim and
Koca, Suleyman Serdar
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Show full item recordAbstract
Objectives: This study aims to examine the effects of sorafenib on a
collagen-induced arthritis (CIA) model.
Materials and methods: The study included 50 randomly selected female
Wistar-albino rats (8-10-week-old, weighing between 200 g to 250 g). The
rats were divided into five equal groups as control, arthritis,
etanercept, sorafenib high-dose, and sorafenib low-dose groups,
respectively. Arthritis was induced by injecting mixed intradermal
chicken type II collagen and incomplete Freund's adjuvant. Twenty-four
hours after the advent of arthritis; rats in group 3 were injected
subcutaneous etanercept (6 mg/kg/week), while those in groups 4 and 5
were given sorafenib (10 or 30 mg/kg/day) orally until they were
sacrificed on the 34th day. The rat claws and trunk bloods were
carefully examined to note perisynovial inflammation and cartilage/bone
injury through histopathology. Tissue vascular endothelial growth factor
(VEGF) and VEGF receptor levels were carefully checked using western
blot analysis.
Results: Analysis of the experimental data showed that CIA decreased in
treatments groups after 12-13 days and 34th day in contrast with the
arthritis group. Histopathological examination revealed broad
perisynovial inflammation and cartilage/bone breakdown in the arthritis
group. Compared to the control group, tissue VEGF and VEGF receptor
levels increased in the arthritis group. Sorafenib and etanercept
decreased tissue VEGF and VEGF receptor levels, perisynovial
inflammation, damage of cartilage/bone.
Conclusion: Our findings indicate that sorafenib treatment ameliorates
CIA with anti-VEGF effectiveness.
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