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find Author "乔珊" 2 results
  • OSAHS和胰岛素抵抗的关系

    目的 研究OSAHS 患者的睡眠呼吸紊乱指标与胰岛素抵抗( IR) 程度的关系。方法 选择OSAHS 患者58 例, 另选57 例非OSAHS患者作为对照。观察经皮血氧饱和度( SpO2 ) , 计算睡眠呼吸暂停低通气指数( AHI) , 次日监测结束后测空腹外周血胰岛素和血糖水平, 采用胰岛素抵抗指数( HOMA-IR) 评估IR 程度。结果 OSAHS 组的HOMA-IR 明显高于非OSAHS 组, OSAHS组平均和最低SpO2 明显低于非OSAHS组。OSAHS 组HOMA-IR 与AHI 呈正相关, 与最低SpO2 呈负相关。结论 OSAHS患者睡眠呼吸功能紊乱与IR 有关, OSAHS可能经IR 这一途径导致心血管疾病

    Release date:2016-09-14 11:23 Export PDF Favorites Scan
  • Neuroprotective effects and mechanisms of selective histone deacetylases inhibitor MS-275 on lithium-pilocarpine induced seizures in rats

    ObjectiveTo investigate the neuroprotective effects and mechanisms of selective histone deacetylases inhibitor MS-275 on rats after seizures. MethodsA total of 75 rats were randomly divided into 5 groups for treatment:control group,pilocarpine group, treatment group Ⅰ(administered with MS-275, 20mg/kg, once a day,intraperitoneally in 7 consecutive days), treatment group Ⅱ(administered with MS-275, 40mg/kg, once a day, intraperitoneally in 7 consecutive days), MS-275 pretreatment group. We used lithium and pilocarpin to induce seizures. Behaviors of rats in each group were observed. At 72 hours after seizures, Nissl staining and immunohistochemical were respectively used to evaluate the loss of neurons and histone acetylation levels of hippocampal CA1 and CA3 regions in each group. Escape latency in the control group, treatment group Ⅰ, treatment group Ⅱ and MS-275 pretreatment group were longer than pilocarpine group(P<0.05). ResultsCompared with the pilocarpine group, rats in MS-275 pretreatment group could delay pilocarpine-induced seizures and reduce mortality (P<0.05). Degree of neuronal loss and degeneration in both treatment group Ⅰ and treatment group Ⅱ were reduced compared with the pilocarpine group (P<0.05) and the level of histone acetylation in hippocampal CA1 and CA3 regions of the rats were increased compared with the pilocarpine group (P<0.05). ConclusionHDACs inhibitors MS-275 can improve the neuronal damage, histone deacetylation of rats' brain and rats cognitive decline, which can exert an neuroprotective effect on rats after seizures, whose mechanism may be related to its antiinflammatory effect.

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