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睾酮在链脲佐菌素诱导的雄性大鼠阿尔茨海默病记忆障碍中的作用。

Role of testosterone in memory impairment of Alzheimer disease induced by Streptozotocin in male rats.

机构信息

Department of pharmacology and toxicology, Tabriz University of Medical Sciences, Tabriz, 51664, Iran.

出版信息

Daru. 2012 Dec 23;20(1):98. doi: 10.1186/2008-2231-20-98.

Abstract

BACKGROUND AND PURPOSE OF THE STUDY

Recent studies demonstrate that androgens, beyond regulating sexual behavior, exert several neuroprotective functions in the brain. The present study was designed to explore effect of testosterone in memory impairment induced by intra- cerebroventricular (icv) injection of streptozotocin (STZ) as a model of sporadic AD.

METHODS

Study was carried out on male Wistar rats. Animals were randomly divided into 11 equal groups. Experimental model of AD was induced by bilateral icv injection of STZ at the dose of 750 μg/Rat/10 μl ACSF at days 1 and 3. STZ-induced memory impairment was assessed two weeks after the last dose of STZ by using a passive avoidance task (1 mA). The interval between the placement of animals in the illuminated chamber and the entry into the dark chamber was measured as a step-through latency (STL). Castration was performed by surgical removing of testis and behavioral study of memory impairment was done after 4 weeks.

RESULTS

Results of this study showed that icv injection of STZ could induce marked (p < 0.05) memory impairment at the dose of 750 μg/Rat/dissolve10 μl CSF/bilateral/days 1 and 3. Therefore, we used this dose of STZ for induction of experimental model of AD. Memory was worsened in castrated rats (P < 0.05) when compared with normal and sham-operated animals. Testosterone replacement therapy (1 mg/kg, sc, for 6 days) in 4 week castrated rats restored memory up to the level of control groups. Testosterone had not any significant effect on memory impairments of non-castrated rats.

MAJOR CONCLUSION

According to the obtained results it can be concluded that testosterone improves cognitive and memory impairment of AD. We suggest that testosterone replacement therapy may have beneficial effect in ameliorating memory impairments of senile patients suffering from AD. Further clinical studies should be carried out to prove possible useful effect of testosterone as an adjuvant therapy in AD.

摘要

背景与研究目的

最近的研究表明,雄激素除了调节性行为外,还在大脑中发挥多种神经保护功能。本研究旨在探讨睾丸酮对侧脑室(icv)注射链脲佐菌素(STZ)诱导的记忆障碍的影响,作为散发性 AD 的模型。

方法

该研究在雄性 Wistar 大鼠中进行。动物被随机分为 11 个相等的组。AD 的实验模型通过双侧 icv 注射 STZ(剂量为 750μg/大鼠/10μl ACSF,第 1 天和第 3 天)诱导。在最后一次 STZ 给药后两周,通过被动回避任务(1 mA)评估 STZ 诱导的记忆障碍。动物放入亮室和进入暗室之间的间隔时间被测量为跨步潜伏期(STL)。通过手术切除睾丸进行去势,在 4 周后进行记忆障碍的行为研究。

结果

本研究结果表明,icv 注射 STZ 可在 750μg/大鼠/10μl CSF/双侧/天 1 和 3 的剂量下诱导明显(p<0.05)的记忆障碍。因此,我们使用这个剂量的 STZ 诱导 AD 的实验模型。与正常和假手术动物相比,去势大鼠的记忆恶化(P<0.05)。4 周去势大鼠给予睾丸酮替代治疗(1mg/kg,sc,连续 6 天)可将记忆恢复至对照组水平。睾丸酮对未去势大鼠的记忆障碍无显著影响。

主要结论

根据获得的结果可以得出结论,睾丸酮可改善 AD 的认知和记忆障碍。我们建议睾丸酮替代治疗可能对改善患有 AD 的老年患者的记忆障碍有益。应进行进一步的临床研究以证明睾丸酮作为 AD 辅助治疗的可能有用效果。

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