首页> 外文期刊>Peptides: An International Journal >NAP has no effect on spatial memory after short-term treatment in advanced stage Alzheimer's disease mouse model.
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NAP has no effect on spatial memory after short-term treatment in advanced stage Alzheimer's disease mouse model.

机译:在晚期阿尔茨海默氏病小鼠模型中短期治疗后,NAP对空间记忆没有影响。

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NAPVSIPQ (NAP) is a small, active fragment of activity-dependent neuroprotective protein that has neuroprotective and memory enhancing properties at very low concentrations. Previous research demonstrated that 1-2 weeks of treatment provided memory enhancing effects in normal middle-aged and cholinergically lesioned rats. Improvement in cognitive performance was shown in 12-month-old C57Bl6/J mice after 10 days of oral treatment with D-NAP and D-SALLRSIPA. Additionally, NAP-related cognitive benefits on spatial memory were observed in a 3xTg Alzheimer mouse model after 6 months of chronic administration at a moderate stage of disease. In this study, the potential memory enhancing effect of NAP was investigated using the APP23 transgenic mouse model for Alzheimer's disease. Twelve-month-old male heterozygous APP23 mice and their wild-type control littermates were intraperitoneally injected with 0.3 microg NAP/g body weight or with saline vehicle for 22 consecutive days. Cognitive performance training in the Morris Water Maze (MWM) started on day 8 of treatment. The internal validity of our study was demonstrated by the fact that the APP23 mice performed significantly worse in the MWM than wild-type animals. Treatment with NAP, however, did not exert any significant effects on MWM performance. Although we failed to show significant memory enhancing effects in this study, NAP might be a promising peptide for disease-modifying therapy in neurodegenerative disease, but short-term effects are probably not to be expected. Also, most likely, treatment should start in an early stage, i.e. before full-blown pathology is eminent, and the necessary treatment period should enclose several months.
机译:NAPVSIPQ(NAP)是活性依赖性神经保护蛋白的小活性片段,在非常低的浓度下具有神经保护和记忆增强特性。先前的研究表明,在正常的中年和胆碱性病变大鼠中,1-2周的治疗可增强记忆力。在用D-NAP和D-SALLRSIPA口服治疗10天后,在12个月大的C57B16 / J小鼠中显示出认知能力的改善。此外,在疾病中期,长期服用6个月后,在3xTg阿尔茨海默病小鼠模型中观察到了NAP相关的空间记忆认知优势。在这项研究中,使用APP23转基因阿尔茨海默氏病小鼠模型研究了NAP潜在的增强记忆作用。连续22天给12个月大的雄性杂合APP23小鼠及其野生型对照同窝小鼠腹膜内注射0.3微克NAP / g体重或生理盐水。在治疗的第8天开始在莫里斯水迷宫(MWM)中进行认知能力训练。 APP23小鼠在MWM中的表现明显比野生型动物差,这一事实证明了我们研究的内部有效性。但是,用NAP进行的治疗对MWM表现没有任何显着影响。尽管我们未能在这项研究中显示出显着的记忆增强作用,但是NAP可能是神经退行性疾病中用于疾病改良疗法的有希望的肽,但是短期作用可能并不在意料之中。而且,最有可能的是,治疗应该在早期阶段开始,即在全面的病理学出现之前,并且必要的治疗期应包括几个月。

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