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find Keyword "局部用药" 2 results
  • 颌面间隙感染脓肿形成后早期穿刺局部用药的疗效观察

    目的观察颌面间隙感染形成脓肿后穿刺吸脓,脓肿内应用庆大霉素冲洗的疗效。 方法对2008年1月-2012年12月收治的形成脓肿的颌面间隙感染患者,按单盲随机分为治疗组(n=32)及对照组(n=30)。治疗组在超声引导下经皮穿刺脓肿,脓腔用庆大霉素冲洗;对照组在超声引导下经皮穿刺吸脓,脓腔内用生理盐水冲洗。比较两种方法治疗后脓肿消失时间、住院时间、疼痛、体温及外周血白细胞恢复正常时间及治疗有效率等。 结果治疗组患者的临床疗效优于对照组(P<0.05);两组患者在治疗后疼痛以及退热时间比较,两组患者差异无统计学意义(P>0.05);两组患者患者治疗期间血常规白细胞降至正常范围时间、住院时间比较,差异有统计学意义(P<0.05)。 结论颌面间隙感染脓肿形成后早期穿刺局部用药有较好疗效。

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  • Study of preventing venous graft restenosis by local application of simvastatin and mechanical preconditioning

    ObjectiveTo investigate the effect of simvastatin and mechanical pretreatment on intimal hyperplasia of venous graft and its mechanism.MethodsTwelve New Zealand rabbits were selected and randomly divided into 4 groups: a blank control group, a simvastatin topical treatment group, a mechanical precondition group and a combined group (n=3 in each group). Ultrasound was used to evaluate the changes of graft wall and blood flow velocity in the graft, and pathological section was used to evaluate the intimal hyperplasia. Human umbilical cord endodermal cells were cultured in vitro. A simvastatin group and a solvent control group were set to detect YAP phosphorylation, downstream target gene expression and cell proliferation.ResultsVascular ultrasound showed that except the simvastatin topical treatment group, the flow velocity in vein grafts in the other three groups significantly increased 21 days after surgery compared with 7 days after surgery (P<0.01). Pathological sections showed that the thickness of new intima in the simvastatin topical treatment group, mechanical precondition group, combined group and blank control group were 45.56±4.11 μm, 201.28±16.71 μm, 143.57±7.82 μm, 249.45±13.33 μm, respectively, and there were statistical differences compared with the blank control group (P<0.05). In vitro results showed that compared with the solvent control group, cell death was observed in high concentration simvastatin (5 mmol/L) group, cell proliferation was inhibited in low concentration simvastatin (2.5 mmol/L) group (P<0.05), the expression of YAP protein in the simvastatin group was unchanged, but the expression of phosphorylated YAP protein significantly increased (P<0.05), and the expression of downstream target gene ccn1 was down-regulated (P<0.001).ConclusionIntravascular local application of simvastatin and mechanical preconditioning alone or in combination can inhibit intimal hyperplasia of venous graft. High concentration of simvastatin has cytotoxicity, while low concentration of simvastatin has inhibitory effect on cell proliferation. Simvastatin can inhibit the formation of new intima by inhibiting the entry of YAP into the nucleus and reducing the transcription of cell proliferation-related target gene ccn1.

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