Effects of exogenous ganglioside-1 on learning and memory in a neonatal rat model of hypoxia-ischemia brain injury

BACKGROUND： Exogenous ganglioside-1 （GM1） can cross the blood-brain barrier and play a protective role against hypoxia-ischemia-induced brain damage. OBJECTIVE： To examine the possible mechanisms of exogenous GM1 protection in hypoxia-ischemia-induced brain damage in a neonatal rat model by measuring changes in brain mass, pathological morphology, growth-associated protein-43 expression, and neurobehavioral manifestations. DESIGN, TIME AND SETTING： A randomized block-design study was performed at the Immunohistochemistry Laboratory of the Pediatric Research Institute, Children＇s Hospital of Chongqing Medical University from August 2005 to August 2006. MATERIALS： A total of 36 neonatal, 7-day-old, Sprague Dawley rats were used in this experiment. The hypoxia-ischemia-induced brain damage model was established by permanently occluding the right carotid artery, followed by oxygen inhalation at a low concentration （8% O2, 92% N2） for 2 hours, METHODS： All rats were randomly divided into the following groups： GMI, model, and sham operation, with 12 rats each group. Rats in the GM 1 and model groups received hypoxic/ischemic-induced brain damage. Rats in the GM1 group received injections of GM1 （i.p., 20 mg/kg） at 0, 24, 48, 72, 96, 120, and 144 hours following models established, and rats in the model group were administered （i.p.） the same amount of saline. The right carotid artery was separated, but not ligated, in the sham operation group rats. MAIN OUTCOME MEASURES： At 1 week after surgery, expression of growth-associated protein-43, a marker of neural development and plasticity, was detected in the hippocampal CA3 region by immunohistochemistry. Brain mass was measured, and the pathological morphology was observed. At 4 weeks after surgery, behavioral changes in the remaining rats were tested by Morris water maze, and growth-associated protein-43 expression was measured. RESULTS： （1） In the GMI and sham operation groups, growth-associated protein-43 expression was greater in the hippocampal CA3 region compared to the model group 1 week after surgery （P 〈 0.05）. In all three groups, brain weight of the right hemisphere was significantly less than the left hemisphere, in particular in the model group （P 〈 0.05）. In the GMI group, the weight difference between two hemispheres, as well as the extent of damage in the right hemisphere, was less than the model group （P 〈 0.01 ）. In the sham operation Uoup, brain tissue consisted of integrated structures and ordered cells. In the model group, the cerebral cortex layers of the right hemisphere were not defined, neurons were damaged, and neurons were disarranged in the hippocampal area. In the GM1 group, neurons were dense in the right cerebral cortex and hippocampal area, with no significant change in glial proliferation. （2） The average time of escape latency in the GM1 group was shortened 4 weeks alter surgery, and significantly less than the model group （P 〈 0.05）. In addition, the frequency platform passing in the GMI group was significantly greater than the model group （P 〈 0.01）. CONCLUSION： Exogenous GM1 may reduce brain injury and improve learning and memory in hypoxia-ischemia-induced brain damage rats. This protection may be associated with increased growth-associated protein-43 expression, which is involved in neuronal remodeling processes.

Effects of Batroxobin on Spatial Learning and Memory Disorder of Rats with Temporal Ischemia and the Expression of HSP32 and HSP70

The effect of Batroxobin on spatial memory disorder of left temporal ischemic rats and the expression of HSP32 and HSP70 were investigated with Morri`s water maze and immunohistochemistry methods. The results showed that the mean reaction time and distance of temporal ischemic rats in searching a goal were significantly longer than those of the sham-operated rats and at the same time HSP32 and HSP70 expression of left temporal ischemic region in rats was significantly increased as compared with the sham-operated rats. However, the mean reaction time and distance of the Batroxobin-treated rats were shorter and they used normal strategies more often and earlier than those of ischemic rats. The number of HSP32 and HSP70 immune reactive cells of Batroxobin-treated rats was also less than that of the ischemic group. In conclusion, Batroxobin can improve spatial memory disorder of temporal ischemic rats; and the down-regulation of the expression of HSP32 and HSP70 is probably related to the attenuation of ischemic injury.

Aminooxyacetic acid improves learning and memory in a rat model of chronic alcoholism

Chronic alcoholism seriously damages the central nervous system and leads to impaired learning and memory.Cell damage in chronic alcoholism is strongly associated with elevated levels of hydrogen sulfide（H2S） and calcium ion overload.Aminooxyacetic acid is a cystathionine-β-synthase activity inhibitor that can reduce H2S formation in the brain.This study sought to observe the effect of aminooxyacetic acid on learning and memory in a chronic alcoholism rat model.Rats were randomly divided into three groups.Rats in the control group were given pure water for 28 days.Rats in the model group were given 6% alcohol for 28 days to establish an alcoholism rat model.Rats in the aminooxyacetic acid remedy group were also given 6% alcohol for 28 days and were also intraperitoneally injected daily with aminooxyacetic acid（5 mg/kg） from day 15 to day 28.Learning and memory was tested using the Morris water maze test.The ultrastructure of mitochondria in the hippocampus was observed by electron microscopy.H2S levels in the hippocampus were measured indirectly by spectrophotometry,and ATPase activity was measured using a commercial kit.The expression of myelin basic protein was determined by immunohistochemistry and western blotting.Compared with the control group,latency and swimming distance were prolonged in the navigation test on days 2,3,and 4 in the model group.In the spatial probe test on day 5,the number of platform crosses was reduced in the model group.Cristae cracks,swelling or deformation of mitochondria appeared in the hippocampus,the hippocampal H2S level was increased,the mitochondrial ATPase activity was decreased,and the expression of myelin basic protein in the hippocampus was down-regulated in the model group compared with the control group.All the above indexes were ameliorated in the aminooxyacetic acid remedy group compared with the model group.These findings indicate that aminooxyacetic acid can improve learning and memory in a chronic alcoholism rat model,which may be associated with reduction of hippocampal H2S level and mitochondrial ATPase activity,and up-regulation of myelin basic protein levels in the hippocampus.

二甲双胍对小鼠脑缺血再灌注损伤后认知功能的影响及其机制

目的探讨二甲双胍对脑缺血再灌注(I/R)小鼠认知功能的影响及其机制。方法采用随机数字表法将40只雄性C57BL/6小鼠[(23±2)g,7~8周龄]分为4组:sham组、I/R组、I/R+100 mg/kg二甲双胍组(低剂量组)和I/R+200 mg/kg二甲双胍组(高剂量组),每组10只。脑缺血组小鼠采用大脑中动脉阻断(MCAO)60 min后再灌注7 d,sham组除不插入细丝阻断外,其余手术步骤相同;低剂量组和高剂量组小鼠在脑缺血再灌注后4 h,每天分别用100,200 mg/kg二甲双胍溶液灌胃,持续7 d。采用Morris水迷宫实验评价小鼠学习和记忆相关指标;采用干湿质量法评估小鼠脑水肿情况;采用HE染色评估小鼠神经元形态变化;采用ELISA试剂盒检测小鼠脑组织脑源性神经营养因子(BDNF)含量和超氧化物歧化酶(SOD)活性。结果与sham组相比,I/R组小鼠自发交替正确率降低,逃避潜伏期增加,目标象限时间降低,穿越平台次数降低(均P<0.05);脑组织含水量增加(P<0.05);BDNF含量和SOD活性均降低(P<0.05);脑组织中变性神经元数量增多。与I/R组相比,低剂量组小鼠目标象限时间增加(P<0.05);高剂量组小鼠自发交替正确率增加(P<0.05),逃避潜伏期降低(P<0.05),目标象限时间增加(P<0.05),穿越平台次数增加(P<0.05),脑组织含水量降低(P<0.05),BDNF含量和SOD活性增加(P<0.05),神经元变性减少。结论200 mg/kg二甲双胍后处理可改善脑缺血再灌注小鼠认知功能,可能与脑水肿减轻、神经元变性改善、脑内BDNF含量和SOD活性增加有关。

An enriched environment increases the expression of fibronectin type Ⅲ domain-containing protein 5 and brain-derived neurotrophic factor in the cerebral cortex of the ischemic mouse brain

Many studies have shown that fibronectin type III domain-containing protein 5(FDNC5) and brain-derived neurotrophic factor(BDNF) play vital roles in plasticity after brain injury. An enriched environment refers to an environment that provides animals with multi-sensory stimulation and movement opportunities. An enriched environment has been shown to promote the regeneration of nerve cells, synapses, and blood vessels in the animal brain after cerebral ischemia;however, the exact mechanisms have not been clarified. This study aimed to determine whether an enriched environment could improve neurobehavioral functions after the experimental inducement of cerebral ischemia and whether neurobehavioral outcomes were associated with the expression of FDNC5 and BDNF. This study established ischemic mouse models using permanent middle cerebral artery occlusion(pMCAO) on the left side. On postoperative day 1, the mice were randomly assigned to either enriched environment or standard housing condition groups. Mice in the standard housing condition group were housed and fed under standard conditions. Mice in the enriched environment group were housed in a large cage, containing various toys, and fed with a standard diet. Sham-operated mice received the same procedure, but without artery occlusion, and were housed and fed under standard conditions. On postoperative days 7 and 14, a beam-walking test was used to assess coordination, balance, and spatial learning. On postoperative days 16–20, a Morris water maze test was used to assess spatial learning and memory. On postoperative day 15, the expression levels of FDNC5 and BDNF proteins in the ipsilateral cerebral cortex were analyzed by western blot assay. The results showed that compared with the standard housing condition group, the motor balance and coordination functions(based on beam-walking test scores 7 and 14 days after operation), spatial learning abilities(based on the spatial learning scores from the Morris water maze test 16–19 days after operation), and memory abilities(based on the memory scores of the Morris water maze test 20 days after operation) of the enriched environment group improved significantly. In addition, the expression levels of FDNC5 and BDNF proteins in the ipsilateral cerebral cortex increased in the enriched environment group compared with those in the standard housing condition group. Furthermore, the Pearson correlation coefficient showed that neurobehavioral functions were positively associated with the expression levels of FDNC5 and BDNF(r = 0.587 and r = 0.840, respectively). These findings suggest that an enriched environment upregulates FDNC5 protein expression in the ipsilateral cerebral cortex after cerebral ischemia, which then activates BDNF protein expression, improving neurological function. BDNF protein expression was positively correlated with improved neurological function. The experimental protocols were approved by the Institutional Animal Care and Use Committee of Fudan University, China(approval Nos. 20160858 A232, 20160860 A234) on February 24, 2016.

Paired associative stimulation improves synaptic plasticity and functional outcomes after cerebral ischemia

Paired associative stimulation is a relatively new non-invasive brain stimulation technique that combines transcranial magnetic stimulation and peripheral nerve stimulation. The effects of paired associative stimulation on the excitability of the cerebral cortex can vary according to the time interval between the transcranial magnetic stimulation and peripheral nerve stimulation. We established a model of cerebral ischemia in rats via transient middle cerebral artery occlusion. We administered paired associative stimulation with a frequency of 0.05 Hz 90 times over 4 weeks. We then evaluated spatial learning and memory using the Morris water maze. Changes in the cerebral ultra-structure and synaptic plasticity were assessed via transmission electron microscopy and a 64-channel multi-electrode array. We measured mRNA and protein expression levels of brain-derived neurotrophic factor and N-methyl-D-aspartate receptor 1 in the hippocampus using a real-time polymerase chain reaction and western blot assay. Paired associative stimulation treatment significantly improved learning and memory in rats subjected to cerebral ischemia. The ultra-structures of synapses in the CA1 area of the hippocampus in rats subjected to cerebral ischemia were restored by paired associative stimulation. Long-term potentiation at synapses in the CA3 and CA1 regions of the hippocampus was enhanced as well. The protein and mRNA expression of brain-derived neurotrophic factor and N-methyl-D-aspartate receptor 1 increased after paired associative stimulation treatment. These data indicate that paired associative stimulation can protect cog-nition after cerebral ischemia. The observed effect may be mediated by increases in the mRNA and protein expression of brain-derived neurotrophic factor and N-methyl-D-aspartate receptor 1, and by enhanced synaptic plasticity in the CA1 area of the hippocampus. The animal experiments were approved by the Animal Ethics Committee of Tongji Medical College, Huazhong University of Science & Technology, China(approval No. TJ-A20151102) on July 11, 2015.

菱角壳提取物对局灶性脑缺血再灌注大鼠学习记忆能力及肌力的作用

探究菱角壳提取物对脑缺血再灌注大鼠学习记忆能力和肌力的作用及机制。成年雄性SD大鼠建立局灶性脑缺血再灌注模型,随机分为假手术组、模型组、菱角壳提取物组,每组8只。给药7 d后,对大鼠进行神经功能缺陷评分、Morris水迷宫定位航行实验和空间探索实验及大鼠四肢肌力测定;同时检测脑组织超氧化物歧化酶(Superoxide Dismutase,SOD)活性及丙二醛(Malondialdehyde,MDA)含量。结果发现,菱角壳提取物组大鼠神经功能缺陷评分2.63分,低于模型组(P<0.05);定位航行实验中,菱角壳提取物组大鼠在平台所在象限停留时间为24.89 s,与模型组相比延长(P<0.05),游泳路程为24084.20 mm,明显增加(P<0.001),成功潜伏期16.22 s和总路程24404.65 mm则显著缩短(P<0.001);空间探索实验中,与模型组相比,大鼠穿越有效区域次数5.75次、在有效区域停留时间22.21 s以及在有效区域游泳路程33744.41 mm均明显增加(P<0.05);菱角壳提取物组大鼠四肢肌力为296.18 N/g,与模型组相比明显增强(P<0.001);大鼠脑组织中SOD活性和MDA含量分别为4.27 NU/mg pro、2.33 nmol/mg pro,与模型组相比,结果亦具有显著性差异(P<0.001)。以上结果表明,菱角壳提取物能明显增强局灶性缺血再灌注大鼠的学习记忆能力和肌力,该作用可能与其减轻自由基损伤有关。

Reduced brain-derived neurotrophic factor expression in cortex and hippocampus involved in the learning and memory deficit in molarless SAMP8 mice

Background The molarless condition has been reported to compromise learning and memory functions. However, it remains unclear how the molarless condition directly affects the central nervous system, and the functional consequences on the brain cortex and hippocampus have not been described in detail. The aim of this study was to find the molecular mechanism related with learning and memory deficit after a bilateral molarless condition having been surgically induced in senescence-accelerated mice/prone8 （SAMP8） mice, which may ultimately provide an experimental basis for clinical prevention of senile dementia.Methods Mice were either sham-operated or subjected to complete molar removal. The animals＇ body weights were monitored every day. Learning ability and memory were measured in a water maze test at the end of the 1 st, 2nd, and 3rd months after surgery. As soon as significantly prolonged escape latency in the molarless group was detected, the locomotor activity was examined in an open field test. Subsequently, the animals were decapitated and the cortex and hippocampus were dissected for Western blotting to measure the expression levels of brain-derived neurotrophic factor （BDNF） and the tropomyosin related kinase B （TrkB）, the high affinity receptor of BDNF.Results Slightly lower weights were consistently observed in the molarless group, but there was no significant difference in weights between the two groups （P〉0.05）. Compared with the sham group, the molarless group exhibited lengthened escape latency in the water maze test three months after surgery, whereas no difference in locomotor activity was observed. Meanwhile, in the cortex and hippocampus, BDNF levels were significantly decreased in the molarless group （P〈0.05）; but the expression of its receptor, TrkB, was not significantly affected.Conclusion These results suggested that the molarless condition impaired learning and memory abilities in SAMP8mice three months after teeth extraction, and this effect was accompanied by significantly reduced BDNF expression in the cortex and hippocampus.

大鼠脑内caveolin-1蛋白的表达及其在分辨学习中的作用

Caveolin-1(Cav-1)蛋白作为细胞质膜结构小窝(caveolae)的标志蛋白,在胆固醇运输、膜组装、信号转导和细胞转化过程中扮演重要的角色。为了探讨Cav-1蛋白在中枢神经系统可塑性及学习记忆中的作用,本文以Sprague-Dawley大鼠为实验对象,利用蛋白质免疫印迹杂交方法观察了Cav-1蛋白在不同年龄大鼠脑内表达的特征,并研究了Y-迷宫训练前后Cav-1蛋白表达的变化。结果表明:(1)大鼠不同脑区Cav-1蛋白表达的年龄特征不同。海马内的表达属青年鼠最高,其次是老年鼠和幼年鼠;皮层内的表达属幼年鼠最高,其次是老年鼠,青年鼠最低;小脑内的表达无明显年龄差异。(2)Y-迷宫训练引起青年鼠海马和前额叶皮层内Cav-1蛋白的表达显著增加。结果提示,Cav-1蛋白与动物脑发育和学习记忆有密切关系,可能参与中枢可塑性的调节。

低氧预适应对大鼠缺血-再灌注性脑损伤中HSP-70、Survivin蛋白和学习记忆能力的影响

目的探讨低氧预适应减轻大鼠缺血-再灌注性脑损伤中学习记忆能力及HSP-70、存活素蛋白表达的变化。方法采用SD大鼠局灶性脑缺血再灌注模型(MCAO),将48只大鼠随机分为3组6个亚组:假手术组、缺血再灌注组(I/R)、低氧预适应组(HP+I/R),应用免疫组织化学法研究脑组织细胞凋亡相关蛋白存活素和应激蛋白HSP-70的表达情况;并通过Y-电迷宫测试缺血再灌注24h后大鼠学习、记忆能力。结果高倍视野下存活素和HSP-70蛋白阳性细胞数比较,HP+I/R组与I/R组及假手术组间差异具有统计学意义(P<0.05)。缺血3h再灌注24h后,Y-电迷宫测试大鼠学习记忆能力,HP+I/R组优于I/R组(P<0.05)。结论低氧预适应可减轻局灶性缺血再灌注脑损伤,提高动物学习记忆能力和损伤后神经功能恢复;上调神经细胞中存活素、HSP-70蛋白表达可能是其发挥保护作用的分子机制之一。

红景天苷预处理对大鼠全脑缺血再灌注后神经行为学的影响

目的:探讨红景天苷预处理对大鼠全脑缺血再灌注后神经行为学的影响及其可能机制。方法:60只SD雄性大鼠随机分为假手术组、模型组及红景天苷预处理组,每组20只。采用四血管阻断法建立全脑缺血再灌注模型。红景天苷预处理组大鼠予腹腔注射红景天苷12mg/(kg·d),连续7d,最后一次给药后30min建立急性全脑缺血再灌注模型。再灌注后24h每组各取5只大鼠,取右侧大脑采用干湿重法计算脑组织含水量;左侧大脑取海马测定超氧化物歧化酶(superoxide dismutase,SOD)活性及丙二醛(malondialdehyde,MDA)含量。每组其余15只大鼠分别于再灌注前及再灌注后6、12、24、48和96h进行神经损害严重程度评分(neurological severity score,NSS);并于再灌注后第5天开始进行Morris水迷宫实验。结果:模型组脑组织含水量、SOD活性、MDA含量、NSS、平均潜伏期及探索实验中在第2象限时间比与假手术组比较差异有统计学意义(P<0.05);红景天苷预处理组与模型组比较,脑含水量降低,SOD活性增高,MDA含量降低,NSS降低,平均潜伏期缩短,第2象限时间比增高,差异有统计学意义(P<0.05)。结论:红景天苷可减轻大鼠全脑缺血再灌注后脑水肿程度,缓解海马区自由基代谢异常,改善认知功能。

川芎嗪对大鼠局部脑缺血后空间学习和记忆的影响

目的探讨川芎嗪对大鼠局部脑缺血后空间学习记忆能力障碍的作用。方法线栓法制作大鼠大脑中动脉阻塞(MCAO)模型,术后2周内腹腔注射川芎嗪,第15天开始采用Morris水迷宫装置评价大鼠的空间学习记忆能力,脑切片尼氏染色观察皮质和海马的神经元数量变化。结果脑缺血对照组大鼠在定向航行试验和空间探索试验中均表现出明显的空间认知功能的障碍,川芎嗪治疗组大鼠平均逃避潜伏期与缺血对照组比较明显缩短(P<0.01)。在空间探索试验中,川芎嗪治疗组大鼠原平台象限停留时间百分比以及穿过原平台位置次数均大于脑缺血对照组(P<0.01)。在形态学观察中,川芎嗪治疗组大鼠缺血侧顶叶皮质神经元数量明显多于脑缺血对照组(P<0.01),各组动物海马神经元数量上无统计学差异。结论川芎嗪可以明显改善大鼠永久性局部脑缺血后空间学习记忆能力,其机制可能与川芎嗪对神经元的保护作用有关。

胞二磷胆碱对大鼠局部脑缺血后空间学习和记忆的影响

目的探讨胞二磷胆碱对大鼠局部脑缺血后空间学习和记忆能力的影响。方法实验分为正常对照组、缺血对照组和胞二磷胆碱组。线栓法制作大鼠大脑中动脉阻塞模型,术后2周内腹腔注射胞二磷胆碱,第15天开始采用Morris 水迷宫装置评价大鼠的空间学习和记忆能力。结果脑缺血对照组大鼠在定向航行试验和空间探索试验中均表现出明显的空间认知功能的障碍,胞二磷胆碱组大鼠平均逃避潜伏期与缺血对照组比较明显缩短(P<0．01)。在空间探索试验中,胞二磷胆碱组大鼠原平台象限停留时间百分比以及穿过原平台位置次数均大于脑缺血对照组(P<0．01)。缺血对照组多采用边缘式和随机式搜索策略;正常对照组多采用直线式和趋向式搜索策略;胞二磷胆碱组采用趋向式和随机式搜索策略的频数较多。结论胞二磷胆碱可以明显改善大鼠永久性局部脑缺血后空间学习和记忆能力。

饮水砷暴露对大鼠血液和脑组织砷蓄积及学习与记忆能力的影响

目的研究饮水砷暴露对大鼠学习与记忆能力的影响。方法将48只雄性健康断乳 SD 大鼠随机分为4组,每组12只。对照组饮用自来水,砷暴露组分别饮用2.72、13.6和68 mg/L 亚砷酸钠溶液。饮水砷暴露12周后,用 Morris水迷宫检测大鼠的学习记忆能力,水迷宫实验完成后用氢化物发生-原子荧光光谱法测定大鼠血砷和脑砷含量。结果血砷含量随饮水砷浓度升高而升高,与对照组相比,差异有统计学意义(P<0.05)。脑砷含量随饮水砷浓度升高而升高,13.6mg/L 和68mg/L 组与对照组相比,差异有统计学意义(P<0.05)。在定向航行实验中,与对照组相比,68mg/L 组大鼠逃逸潜伏期显著延长(P<0.05)。在空间探索实验和可视平台实验中,各组间差异没有统计学意义。结论相对较高剂量的饮水砷暴露能降低大鼠的学习能力。

黑木耳多糖对抗大鼠慢性缺血性脑损伤

目的:观察黑木耳多糖(AAP)对大鼠慢性脑缺血损伤的保护作用,并探讨其相关机制。方法:雄性成年SD大鼠右侧永久性大脑中动脉栓塞(MCAO),建立慢性脑缺血模型,缺血后每天分别给予不同浓度的AAP灌胃4周。银杏叶提取物作为阳性对照。4周后采用Morris水迷宫检测大鼠学习记忆能力。取脑做冰冻切片进行Nissl染色,观察存活神经元数量,并测定脑组织丙二醛(MDA)水平和超氧化物歧化酶(SOD)活性。结果:AAP能明显改善脑缺血大鼠的学习记忆能力,增加海马神经元的存活数量,并且能够使脑组织长期MCAO诱导的MDA生成减少,使SOD活性显著升高。高剂量AAP(200mg/kg)的作用和银杏叶提取物相比更明显。结论:AAP明显减轻大鼠慢性脑缺血损伤,其作用与其对抗过氧化应激有关。

丙泊酚对新生鼠神经干细胞增殖及学习记忆的影响

目的研究丙泊酚对新生鼠神经干细胞增殖及学习记忆的影响。方法出生后7 dWistar乳鼠104只随机均分成四组:丙泊酚50 mg/kg组(A组)、丙泊酚100 mg/kg组(B组)、生理盐水10 ml/kg组(C组)、脂肪乳剂10 ml/kg组(D组),各组均为腹腔注射,连续注射7 d,第7天每组取10只腹腔注射300 mg/kg 5-溴脱氧尿苷(Brdu),12 h后灌注切脑片做Brdu免疫组化,6只取海马提蛋白westerblot检测脑源性神经营养因子(BDNF),剩下10只饲养2个月后行Morris水迷宫测试。结果与C组比较,D组对Brdu阳性细胞无影响,A、B组Brdu阳性细胞数明显减少(P<0.05),其中B组阳性细胞数又明显少于A组(P<0.05)。A、B组BDNF含量减少,但只有B组明显抑制成年后鼠的学习记忆功能。结论丙泊酚能抑制新生鼠神经干细胞增殖,大剂量丙泊酚可损害鼠成年后学习记忆功能,可能与丙泊酚减少BDNF分泌有关。

瑞芬太尼预处理对短暂脑缺血后大鼠学习记忆能力的影响

目的观察瑞芬太尼预处理对短暂脑缺血后大鼠学习与记忆能力的影响,并进一步探讨其作用机制。方法♂SD大鼠40只,随机分为假手术(Sham)组、模型(Model)组、瑞芬太尼预处理低剂量(RPC1)、中剂量(RPC2)和高剂量(RPC3)组,每组8只。采用两侧颈总动脉夹闭8min加放血性低血压(30～35mmHg)模型,实现大鼠短暂性全脑缺血,瑞芬太尼预处理分别以0.2、0.6和2μg·kg-1.min-1速率尾静脉泵注5min,停止5min,重复进行3次。再灌注3d后利用Morris水迷宫测量术后大鼠空间学习与记忆的能力,用免疫组织化学法测定大鼠海马CA1区胆碱乙酰转移酶(cho-line acetyltransferase,ChAT)的表达。结果瑞芬太尼中、高剂量组和假手术组大鼠的潜伏期明显短于模型组(P<0.05),在记忆保留实验,瑞芬太尼中、高剂量组和假手术组大鼠的靶象限时间百分比明显高于模型组(P<0.05),而海马CA1区ChAT的表达中剂量、高剂量组也明显高于模型组(P<0.05)。结论瑞芬太尼预处理对短暂脑缺血后大鼠学习与记忆能力有明显改善作用,其作用机制可能与ChAT表达上调有关。

学习记忆训练对全脑缺血大鼠认知能力的影响及其胆碱能机制

目的：探讨学习记忆训练对全脑缺血大鼠空间学习记忆能力的影响及其胆碱能机制。方法：选用健康雄性SD大鼠90只随机分为假手术组、对照组、训练组。采用改良Pulsinelli’s 4血管闭塞法制作全脑缺血大鼠模型。术后1周以Y型电迷宫训练大鼠，分别在训练7d、14d、21d后应用Y型电迷宫检测比较i组大鼠的空间学习记忆能力的差异。结果：训练21d后，对照组与假手术组和训练组比较，Y型电迷宫全天总反应时间和潜伏期明显延长（P〈0.05），错误反应次数明显增多（P〈0.05）。对照组神经元明显水肿，细胞器明显减少。训练组神经元细胞大、圆，细胞质丰富。对照组CA1区乙酰胆碱转移酶的光密度值明显低于假手术组和训练组（P〈0.05），而训练组和假手术组之间差异无显著性意义（P〉0.05）。结论：学习记忆训练可以改善全脑缺血大鼠的空间学习记忆能力，其机制可能是训练增加了乙酰胆碱转移酶的活性或训练抑制了乙酰胆碱转移酶活性的降低。

脑细胞活性因子对小鼠学习、记忆能力的影响

目的 观察脑细胞活性因子 (BCAF)对小鼠学习、记忆能力提高和改善的作用。方法 通过改良的Morris水迷宫法测试4月龄小鼠 ,并将其分为学习记忆障碍组 (A、B) ,学习记忆减退组 (C、D) ,学习记忆正常组 (E、F) ,以及学习记忆正常加东莨菪碱组(G、H)。每组均设BCAF治疗组 (B、D、F、H)与生理盐水 (NS)对照组 (A、C、E、G)。治疗 14天后 ,再次水迷宫测试小鼠定向航行能力。结果 ①BCAF治疗组 :B、D和F组治疗后平均逃避潜伏期明显缩短 ,治疗前后比较差异十分显著 (均为P <0 .0 0 1)。②NS对照组 :A、C和E组治疗前后平均逃避潜伏期无显著差异 (分别为P >0 .5 ,P >0 .2和P >0 .2 )。③NS的A组与BCAF的B组治疗后比较差异显著 (P <0 .0 2 )。④BCAF加东莨菪碱治疗组 (H组 )与NS加东莨菪碱对照组 (G组 )一样 ,各组治疗前后平均逃避潜伏期比较均无显著差异 (P >0 .2和P >0 .1)。结论 BCAF可提高和改善小鼠学习记忆能力 。

养血清脑颗粒对慢性脑缺血大鼠脑血流量及认知功能的影响

目的：观察养血清脑颗粒(YQG)对慢性脑缺血大鼠脑血流量及认知功能的影响。方法：Wistar大鼠双侧颈总动脉永久结扎造成慢性脑缺血模型,激光多普勒血流仪检测额叶皮质局部脑血流量；Morris水迷宫检测认知功能。结果：术后模型组大鼠脑血流量骤降,并呈慢性持续下降趋势(P＜0．05)；大鼠出现认知功能障碍,隐匿平台逃避潜伏期和游泳距离明显延长(P＜0．05,P＜0．01),空间探索实验逃避潜伏期明显延长,穿越次数明显减少(P＜0．01),平台象限游泳时间和距离均缩短(P＜0．01)。YQG 3个剂量组均能明显增加脑血流量,改善认知障碍(P＜0．05或P＜0．01)。结论：YQG能明显改善慢性脑缺血大鼠局部脑血流量,提高学习记忆能力,有随疗程的增加而作用增强的趋势。