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Polyethylene glycol administration in an animal model of focal ischemic stroke.

机译:在局灶性缺血性中风的动物模型中施用聚乙二醇。

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摘要

In the United States alone, approximately 700,000 people will suffer a first or recurrent stroke this year. Of those, approximately 275,000 will die, making stroke America's third largest killer. Further, stroke is a leading cause of adult disability with survivors experiencing sensory, motor, and cognitive deficits that can lead to a lack of independence and a reduced quality of life. Here, we test whether polyethylene glycol (PEG), a biocompatible polymer used successfully in other injury models, can promote anatomical and behavioral recovery from focal cerebral ischemia (i.e., stroke) when administered two hours following middle cerebral artery occlusion (MCAo). Behavior was assessed using a rotarod apparatus and an open-field exploration box. Additionally, the ischemic lesion was quantified following histological staining by triphenyltetrazolium chloride (TTC), and a viable cell count was determined utilizing the MTT assay.;Based on the behavioral data, no clear conclusion can be discerned. Independently, the rotarod data suggest that PEG was successful. With the exception of day 2, the PEG-treated animals displayed superior performance for both top speed and time in comparison to injured, control animals. By day 7, the differences between groups were significant. However, results from the exploration box question the usage of PEG as administered. Across all measures (e.g., total beam breaks, distance traveled), uninjured animals performed significantly better than injured animals, regardless of drug treatment or time of testing (light vs. dark cycle). The injured, PEG-treated and injured, control animals did not differ significantly.;Results of the histological examination demonstrate that a significant difference in ischemic volume existed between PEG-treated and control animals, with the PEG-treated animals exhibiting more ischemia. Further, a comparison of percent ischemia between injured groups revealed a nearly significant difference. Finally, comparisons between adjusted absorbances and percent adjusted absorbances for injured tissues, as quantified by the MTT assay, revealed no significant differences between treatment groups.;Together, the results demonstrate that PEG administration, at the given dosage and time, did not significantly advance anatomical or behavioral recovery, with the exception of the rotarod data. Thus, PEG does not appear to afford considerable neuroprotection within the experimental parameters of this MCAo injury model.
机译:仅在美国,今年就有约700,000人患有中风或中风。其中约有275,000人将死,成为中风美国的第三大杀手。此外,中风是成人残疾的主要原因,幸存者会出现感觉,运动和认知缺陷,这可能导致缺乏独立性和生活质量下降。在这里,我们测试了在中脑动脉闭塞(MCAo)后两小时给药的聚乙二醇(PEG)(一种在其他损伤模型中成功使用的生物相容性聚合物)是否能促进从局灶性脑缺血(即中风)的解剖和行为恢复。使用旋转仪和开放野外探测箱评估行为。另外,通过组织学染色通过氯化三苯基四唑鎓(TTC)对缺血性损伤进行定量,并使用MTT测定法确定活细胞计数。;基于行为数据,无法辨别清楚的结论。独立地,旋转数据表明PEG成功。与受伤的对照动物相比,除第2天外,PEG处理的动物在最高速度和时间上均表现出优异的性能。到第7天,两组之间的差异显着。然而,来自探索盒的结果对施用PEG的用法提出了质疑。在所有衡量指标(例如总光束中断,行进距离)中,无论药物治疗或测试时间如何(光周期与暗周期),未受伤的动物的表现均明显优于受伤的动物。受伤的,经PEG处理的动物和受伤的对照动物没有显着差异。;组织学检查结果表明,在PEG处理的动物和对照动物之间,缺血体积存在显着差异,其中PEG处理的动物表现出更多的局部缺血。此外,比较受伤组之间的局部缺血百分率显示出几乎显着的差异。最后,通过MTT测定法定量比较受伤组织的调整后的吸光度和调整后的吸光度百分比,结果显示各治疗组之间无显着差异。总而言之,结果表明,在给定的剂量和时间下,PEG给药并没有明显进展。解剖或行为恢复,但轮转数据除外。因此,在该MCAo损伤模型的实验参数范围内,PEG似乎没有提供明显的神经保护作用。

著录项

  • 作者

    Altizer, Alicia M.;

  • 作者单位

    Purdue University.;

  • 授予单位 Purdue University.;
  • 学科 Biology Neuroscience.
  • 学位 Ph.D.
  • 年度 2006
  • 页码 144 p.
  • 总页数 144
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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