首页> 外文期刊>Journal of Neuroscience Research >Comparing the effect of the novel ionic cocrystal of lithium salicylate proline (LISPRO) with lithium carbonate and lithium salicylate on memory and behavior in female APPswe/PS1dE9 Alzheimer's mice
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Comparing the effect of the novel ionic cocrystal of lithium salicylate proline (LISPRO) with lithium carbonate and lithium salicylate on memory and behavior in female APPswe/PS1dE9 Alzheimer's mice

机译:比较锂水杨酸锂脯氨酸(LISPRO)与碳酸锂和锂水杨酸锂对雌性Appswe / PS1DE9 Alzheimer小鼠锂水杨酸锂的影响

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摘要

Abstract Alzheimer's disease (AD) is characterized by progressive decline of cognition and associated neuropsychiatric signs including weight loss, anxiety, depression, agitation, and aggression, which is particularly pronounced in the female gender. Previously, we have shown that a novel ionic co‐crystal of lithium salicylate proline (LISPRO) is an improved lithium formulation compared to the carbonate or salicylate form of lithium in terms of safety and efficacy in reducing AD pathology in Alzheimer's mice. The current study is designed to compare the prophylactic effects of LISPRO, lithium carbonate (LC), and lithium salicylate (LS) on cognitive and noncognitive impairments in female transgenic APPswe/PS1dE9 AD mice. Female APPswe/PS1dE9 mice at 4?months of age were orally treated with low‐dose LISPRO, LS, or LC for 9?months at 2.25?mmol lithium/kg/day followed by determination of body weight, growth of internal organs, and cognitive and noncognitive behavior. No significant differences in body or internal organ weight, anxiety or locomotor activity were found between lithium treated and untreated APPswe/PS1dE9 cohorts. LISPRO, LC, and LS prevented spatial cognitive decline, as determined by Morris water maze and depression as determined by tail suspension test. In addition, LISPRO treatment was superior in preventing associative memory decline determined by contextual fear conditioning and reducing irritability determined by touch escape test in comparison with LC and LS. In conclusion, low‐dose LISPRO, LC, and LS treatment prevent spatial cognitive decline and depression‐like behavior, while LISPRO prevented hippocampal‐dependent associative memory decline and irritability in APPswe/PS1dE9 mice.
机译:摘要Alzheimer的疾病(AD)的特点是认知和相关神经精神症状的逐步下降,包括减肥,焦虑,抑郁,搅动和侵略,这在女性性别中特别明显。以前,我们已经表明,与碳酸锂或锂的水杨酸酯形式的锂在阿尔茨海默氏症小鼠中降低了广告病理学方面,新型离子共晶二晶体(LISPRO)是一种改进的锂制剂。目前的研究旨在比较Lispro,碳酸锂(LC)和水杨酸锂(LS)对雌性转基因Appswe / PS1DE9 AD小鼠的认知和非认知损伤的预防效果。女性Appswe / ps1de9小鼠在4?月龄的年龄,用低剂量的Lispro,LS或LC口服治疗9?月份在2.25?mmol锂/ kg /天,然后测定体重,内脏的生长,和认知和非认知行为。在锂处理和未处理的Appswe / PS1DE9队列之间发现身体或内部器官重量,焦虑或运动活性没有显着差异。 LISPRO,LC和LS防止了空间认知下降,如摩根水迷宫和抑郁由尾悬浮试验确定的。此外,LisPro处理在防止通过语境恐惧调节和降低通过LC和LS比较的触摸逃逸试验确定的烦躁下降的缔合记忆下降的优异情况优异。总之,低剂量的LISPRO,LC和LS治疗防止了空间认知下降和抑郁症状的行为,而LISPRO则在APPSWE / PS1DE9小鼠中阻止了海马依赖的关联记忆下降和烦躁。

著录项

  • 来源
    《Journal of Neuroscience Research》 |2019年第9期|共15页
  • 作者单位

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Neurosurgery &

    Brain Repair Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Neurosurgery &

    Brain Repair Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

    Department of Psychiatry &

    Behavioral Neurosciences Morsani College of MedicineUniversity of South;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 神经病学;
  • 关键词

    Alzheimer's disease; cognitive impairment; depression; irritability; transgenic mice;

    机译:阿尔茨海默病;认知障碍;抑郁症;烦躁;转基因小鼠;

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