| Objective:The chemical formular of BRD is C18H29N3O2,which is a new Roxatidine derivate(The chemical formular is C17H26N2O3) from the revised and modified Acetid Roxatiding.It is a new H2-recepton imtagonist that first combined by us in the world and reported by CA.Test shows the compound has comparaci linger lipid solubility and stronger imtiacid effect compared with RD.The related researches on pharmcological action and it is system has not been reported at home on abroad. Apoptosis plays an important control role in the recovery of the ulcer through the system research on the pharmacological effect and it is system of the new compound ,we want to find its pharmcological action and the molecular action system against gastric ulcer.The research of the project may fill the blank of how BRD defense gastric ulcer both in and outside China,and provide valuable research proof for exploiting new and effective H2-receptor antagonist. Method:1. Divide the animals into groups and prepare a acetic acid injured A-rat model.2. Observe the change of behavion and the ulcer morphology afare A-rat affer given medicine.3. Measure the SOD dose in the serum and gastric tissue of A-rat though Biochemical method.4. Measure the dose of MDA in the serum and gastric tissue of A-rat though Biochemical method.5. Measure the apoptosis of the ulcer mucosa cell though TUNEL method.6. Measure the protein expression of apoptosis inhibiting gene Bcl-2 though immunity combination and chemical method.Result:1.BRD promotes the recovery of the ulcered rat,improve its symptoms of tireness,languidness and hypersomnia,alleviates its histological and pathological injury.2.The dose messuremert of SOD and MDA in the rat's serum and gastric tissue shows,large and small close of BRD both promote the SOD in its serum and gastric tissue,bring down the MDA,and depend on the dose,P<0.01-0.05 compared with the control group.3.The protein expression measure of the apoptosis inhibiting gene Bcl-2 shows BRD could inhibit the aptosis of the gastric mucosa cell and decrease AI,P<0.01-0.05compared with control group.BRD promotes Bcl-2 increase of the mucosa cell;as a result,over-apoptosis is inhibited and mucosa injury is alleviated.Discussion:It has proved that the loss of gastric mucosa epithelium was mainly through apoptosis instead of amotic and the integration of gastric mucosa depends on the balance between cell multiple and cell loss. Grastric ulcer is mainly related to the defensive factors and injure factors of the gastric mucosa.Loss of gastric mucosa epithelium is mainly throuph apoptosis.The experiment proves that BRD promotes protein expression,inhibit apoptosis of the gastric mucosa cell,decrease ulcer index and accelerate ulcer recovery.Radical are toxic product by the organism and injury the servers,It could indute lipid peroxidation effect and produce lipid peroxidation,of with MDA is the most toxious.SOD and MDA could indirectly reflect radical metabolism level.The test shows,BRD could promote SOD level , decrease MDA level , so radicals eliminated,surplus superoxide anions which couse the injury of mucosa reduced,all these suggest that the medicine would improve the ability of antioxidation and eliminating radicals,inhibiting lipid peroxidation anf improving radical metabolism.The tset proves that BRD could promote the recovery of the rat's gastric ulcer mucosa induced by aceric acid and effectively prevent the incidence and development of gastric ulcer.All these results proviod reliable test basis for treating peptic ulcer.Conclusion:BRD could promote the recvery of the rat's gastric ulcer,improve the rat's tireness,languidness,hypersomnia symptoms,alleviate its histological and pathological injury the rat's gastric ulcer mucosa.Promote SOD and decease MDA in the rat's serum and gastric tissue,inhibit apoptosis of the mucosa cell,strengthen the Bcl-2 expression of its mucosa cell.As a result,it inhibit the over-apoptosis of the cell,alleviate the gastric mucosa injury and actively prevented the incidence of getting ulcer or being developed.
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