XIAO Zhi-bin, LIU Xiao-lei, CHENG Ri-qing, et al. Influence of -sitosterol on Gastric Mucosal Side Effect Induced by Aspirin and Its Pharmacological Functions[J]. Chinese journal of experimental traditional medical formulae, 2016, 22(1): 148-152.
DOI:
XIAO Zhi-bin, LIU Xiao-lei, CHENG Ri-qing, et al. Influence of -sitosterol on Gastric Mucosal Side Effect Induced by Aspirin and Its Pharmacological Functions[J]. Chinese journal of experimental traditional medical formulae, 2016, 22(1): 148-152. DOI: 10.13422/j.cnki.syfjx.2016010148.
Influence of -sitosterol on Gastric Mucosal Side Effect Induced by Aspirin and Its Pharmacological Functions
Objective: To study the effect of β-sitosterol on gastric mucosal injury induced by aspirin and its possible mechanism
and explore the effect of β-sitosterol on pharmacological functions of aspirin. Method: Gastric mucosa injury modelsinduced by aspirinin SD rats was established by intragastric administration of different dosesof β-sitosterol(50
150
250 mg·kg-1) for seven days
and ulcer area was assessed to analyze the effect of β-sitosterol on gastric mucosal injury induced by aspirin in rats. Serum superoxide dismutase(SOD)
tumor necrosis factor-α(TNF-α)
prostaglandin E2(PGE2)
malondialdehyde(MDA) and nitric oxide(NO) were measured to analyze the possible mechanism. Rat paw edema test
mouse ear swelling
rat yeast-induced fever test and mouse hot plate test
and platelet aggregation in rats were used to examine the pharmacological effect of different doses of β-sitosterol on anti-inflammatory
antipyretic
analgesic
and inhibition of platelet aggregation induced by aspirin. Result: Compared with aspirin-treated group
gastric ulcer area of β-sitosterol group rats was significantly reduced(P<0.05);gastric ulcer area in the high and middle dose β-sitosterol group rats was significantly smaller than that in β-sitosterol low dose group(P<0.05). Compared with aspirin-treated group
NO and SOD in serum of β-sitosterol rats increased significantly(P<0.05)
TNF-α
MDA significantly decreased(P<0.05)
and PGE2 level was not significantly different. Compared with the model group
toe swelling of rats and ear swelling of micein various treatment groups were significantly reduced(P<0.05);compared with the aspirin-treated group
toe swelling of rats and ear swelling of mice in β-sitosterol group were significantly reduced(P<0.05)
but there is no significant differences between the β-sitosterol groups. Compared with aspirin-treated group
the change in the value of the rectal temperature and pain threshold in mice and platelet aggregation rate in rat of the corresponding β-sitosterol group were no significant difference. Conclusion: β-sitosterol can reduce the aspirin-mediated gastric mucosal injury
and its mechanism may be related to enhancing the clearance capacity of oxygen free radicals(OFR) of body
improving levels of NO
inhibiting aggregation and release of inflammatory cytokines TNF-α;β-sitosterol can enhance the anti-inflammatory effects of aspirin and have no significant effect on antipyretic
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