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首页> 外文期刊>Journal of Molecular Neuroscience: MN >Evaluation of the Effect of Prazosin Treatment on alpha-2c Adrenoceptor and Apoptosis Protein Levels in the Predator Scent-Induced Rat Model of Post-Traumatic Stress Disorder
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Evaluation of the Effect of Prazosin Treatment on alpha-2c Adrenoceptor and Apoptosis Protein Levels in the Predator Scent-Induced Rat Model of Post-Traumatic Stress Disorder

机译:评价普罗唑汀治疗对血糖诱导的后创伤后应力障碍大鼠模型中α-2C肾上腺素受体和凋亡蛋白水平的影响

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The predator scent-induced (PSI) stress model is a rat model used to mimic post-traumatic stress disorder (PTSD) symptoms in humans. There is growing evidence that prazosin, which blocks alpha-1 and is approved by the FDA as an anti-hypertensive drug, can potentially be of use in the treatment of PTSD-related sleep disorders. The aim of this study was to investigate the role of prazosin treatment on behavioral parameters (freezing time, total transitions, and rearing frequency measured from the open field; anxiety index, total entries and time spent in open arms calculated from the elevated plus maze), apoptotic proteins and alpha-2c-AR in fear memory reconsolidation in the PSI stress rat model. We used western blot analysis to determine the effect of prazosin (0.5 mg/kg/ip) on alpha-2c-AR and apoptotic protein expression changes in the frontal cortex, hippocampus, and amygdala. It was determined that in the stress group, there was increased freezing time and anxiety index, and decreased rearing frequency, total transitions, total entries, and time spent in open arms compared to the control groups. Following PSI-stress, pro-apoptotic (bax) protein expression levels increased and alpha-2c AR and anti-apoptotic protein (bcl-2) levels decreased in investigated all brain regions. The majority of stress-induced changes were recovered with prazosin treatment. The results of our study may potentially be useful in understanding the effect of prazosin treatment, given the fact that the amygdala, frontal cortex, and hippocampus regions are affected for stress conditions.
机译:捕食者气味诱导的(PSI)应力模型是用于模拟人后创伤后应激障碍(PTSD)症状的大鼠模型。普拉佐汀的证据越来越多的证据表明,α-1并被FDA批准作为抗高血压药物,可能是在治疗PTSD相关的睡眠障碍中使用的。本研究的目的是探讨普拉索辛治疗对行为参数(冻结时间,总转换和从开放场测量的饲养频率的作用;焦虑指数,在升高的加迷宫中计算的开放式臂中所花费的总条目和时间) ,凋亡蛋白和α-2C-AR在PSI应力大鼠模型中的恐惧记忆再溶解。我们使用Western印迹分析来确定普罗唑汀(0.5mg / kg / IP)对α-2C-AR和凋亡蛋白表达在额叶,海马和杏仁醛的变化的影响。确定在应力组中,与对照组相比,在应力组中,冻结时间和焦虑指数,并降低了饲养频率,总转变,总条目和在张开臂中花费的时间。在psi-ressure,促凋亡(Bax)蛋白表达水平增加和α-2C AR和抗凋亡蛋白(Bcl-2)水平降低,调查所有脑区。大部分压力诱导的变化用普拉索辛治疗回收。我们的研究结果可能潜在可用于了解吡唑嗪治疗的影响,因为杏仁达拉,正面皮质和海马区域受到压力条件的影响。

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