红细胞生成素对海人酸致大鼠认知功能影响及作用机制被引量：1

Effects and mechanism of erythropoietin on the cognitive function of kainic acidinduced epileptic rats

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摘要目的探讨红细胞生成素对海人酸致模型大鼠癫发作及空间学习和记忆能力的影响。方法共96只Sprague-Dawley大鼠随机分为4组,观察不同处理组大鼠行为学变化,Morris水迷宫实验定位航行实验和空间探索实验评价大鼠空间学习和记忆能力,Western blotting法检测大鼠海马组织p38有丝分裂原激活蛋白激酶(p38MAPK)、c-Myc和caspase-3表达变化。结果红细胞生成素组大鼠癫发作程度减轻(P=0.000)。与模型组相比,红细胞生成素低、高剂量组大鼠逃避潜伏期缩短(P=0.043,0.000),第1象限停留时间延长(P=0.000,0.000),穿越平台次数增加(P=0.000,0.046),并以高剂量组显著(均P=0.000);而且,大鼠海马组织p38MAPK(P=0.000,0.000)、c-Myc(P=0.009,0.000)和caspase-3(P=0.003,0.000)表达水平降低,并以高剂量组明显(P=0.040,0.030,0.048)。结论红细胞生成素可以减轻大鼠癫发作程度,提高大鼠空间学习和记忆能力,其作用机制可能与红细胞生成素抑制p38MAPK及其下游c-Myc和caspase-3表达,最终减少神经元凋亡有关。 ObjectiveTo observe the effects of erythropoietin（EPO） on the behaviors and abilitiesof spatial learning and memory of kainic acid（KA）-induced epileptic rats.MethodsA total of 96 ratswere randomly divided into 4 groups： control group, model group, low-dose EPO pretreated group and high-dose EPO pretreated group. After treatment with relevant reagents, the behaviors of rats in each group wereobserved. The abilities of spatial learning and memory were evaluated by Morris water maze test.Expressions of apoptosis- related factors： p38 MAPK, c- Myc and caspase- 3 were detected by Westernblotting.ResultsBehavior observation showed seizures in EPO groups reduced（P = 0.000）. Comparedwith model group, rats in EPO groups had significantly reduced escape latency in positioning navigationtrial（P = 0.043, 0.000）, significantly prolonged first quadrant latency（P = 0.000, 0.000） and increasedplatform crossing index in spatial probe trial（P = 0.000, 0.046）, expressly in high-dose EPO group（P =0.000, for all）. Expressions of p38MAPK（P = 0.000, 0.000）, c-Myc（P = 0.009, 0.000） and caspase-3（P =0.003, 0.000） in rat hippocampus were significantly decreased in EPO groups than that in model group,expressly in high-dose EPO group（P = 0.040, 0.030, 0.048）.ConclusionsErythropoietin can reduce theattack of epileptic rats and increase the ability of spatial learning and memory in KA-induced epileptic rats.The mechanism may be associated with depressing the expression of p38 MAPK and downstream c-Myc andcaspase-3, finally reducing neuronal apoptosis.

作者赫鹏郭金刚

机构地区辽宁省阜新市中心医院神经内科辽宁医学院研究生学院

出处《中国现代神经疾病杂志》 CAS 2015年第5期401-405,共5页 Chinese Journal of Contemporary Neurology and Neurosurgery

关键词红细胞生成素癫红藻氨酸认知障碍海马疾病模型动物 Erythropoietin Epilepsy Kainic acid Cognition disorders Hippocampus Disease models animal

分类号 R741 [医药卫生—神经病学与精神病学]

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