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尼卡地平、氟桂利嗪、利多氟嗪和尼莫地平对蒙古沙鼠海马缺血性损伤的比较保护作用。

Comparative protective effects of nicardipine, flunarizine, lidoflazine and nimodipine against ischaemic injury in the hippocampus of the Mongolian gerbil.

作者信息

Alps B J, Calder C, Hass W K, Wilson A D

机构信息

Department of Pharmacology, Syntex Research Centre, Riccarton, Edinburgh.

出版信息

Br J Pharmacol. 1988 Apr;93(4):877-83. doi: 10.1111/j.1476-5381.1988.tb11475.x.

Abstract
  1. Morphological changes characterizing delayed neuronal death (DND) of selectively vulnerable CA1 pyramidal cells in the hippocampus of the Mongolian gerbil brain occurred 72 h after transient (5 min) bilateral occlusion of the common carotid arteries. 2. Different groups of animals were treated 15 min before carotid artery occlusion and twice daily during the 72 h post-ischaemia period with either saline alone, nicardipine, flunarizine, lidoflazine or nimodipine at doses of 500 micrograms kg-1 intraperitoneally. 3. At 72 h the animals were killed and their brains examined histologically. Absolute cell counts were made from 5 sites distributed linearly throughout the hippocampal CA1 subfield in each hemisphere to determine the percentage DND in each group. Normal brains and those of sham-operated animals were included in the study for comparison. 4. Features of DND were distributed evenly throughout the CA1 subfield in both hemispheres in all groups of gerbils. Nicardipine, lidoflazine and flunarizine, but not nimodipine, were protective. This protection extended linearly throughout the hippocampus without altering the pattern of neuronal damage. 5. Compared to saline-treated (78.3 +/- 2.9% DND) and nimodipine-treated (76.5 +/- 3.4% DND) gerbils, the overall protection afforded by nicardipine (41.8 +/- 3.8% DND) was statistically significant. The effects of lidoflazine (53.6 +/- 7.1%) and flunarizine (55.8 +/- 3.9% DND) were of borderline significance. 6. Abnormal neurones appeared in normal and sham-operated brains to the extent of 4.5 +/- 1.0% and 4.6 +/- 0.4%, respectively. Such changes can be attributed to fixation artefacts. 7. The results demonstrate that overall protection is conferred on ischaemic hippocampal CA1 neurones by nicardipine and to a lesser extent by flunarizine and lidoflazine, but not by nimodipine.
摘要
  1. 蒙古沙鼠脑海马中选择性易损的CA1锥体细胞延迟性神经元死亡(DND)的形态学变化发生在双侧颈总动脉短暂(5分钟)闭塞72小时后。2. 不同组动物在颈动脉闭塞前15分钟接受治疗,并在缺血后72小时内每天两次腹腔注射500微克/千克的生理盐水、尼卡地平、氟桂利嗪、利多氟嗪或尼莫地平。3. 72小时后处死动物,对其大脑进行组织学检查。从每个半球海马CA1亚区线性分布的5个部位进行绝对细胞计数,以确定每组的DND百分比。研究纳入正常大脑和假手术动物的大脑作为对照。4. 在所有沙鼠组中,DND特征在两个半球的CA1亚区均均匀分布。尼卡地平、利多氟嗪和氟桂利嗪具有保护作用,而尼莫地平没有。这种保护作用在整个海马中呈线性延伸,而不改变神经元损伤模式。5. 与生理盐水处理组(DND为78.3±2.9%)和尼莫地平处理组(DND为76.5±3.4%)的沙鼠相比,尼卡地平提供的总体保护作用(DND为41.8±3.8%)具有统计学意义。利多氟嗪(53.6±7.1%)和氟桂利嗪(55.8±3.9% DND)的作用具有临界意义。6. 正常大脑和假手术大脑中出现异常神经元的比例分别为4.5±1.0%和4.6±0.4%。这种变化可归因于固定假象。7. 结果表明,尼卡地平对缺血海马CA1神经元具有总体保护作用,氟桂利嗪和利多氟嗪也有一定程度的保护作用,而尼莫地平则没有。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f93/1853888/157d6d9dbdf1/brjpharm00293-0163-a.jpg

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