创伤后应激障碍对慢性不可预见性应激抑郁模型的影响

目的:观察创伤后应激障碍(PTSD)对慢性不可预见性应激(CUS)抑郁模型的影响。方法:采用足底电击的方法建立大鼠创伤后应激障碍模型。成年雄性S-D大鼠40只随机分为四组(n=10):对照组(C组)、PTSD组、CUS组、PTSD+CUS组(P+C组)。在1、7、14、21天测量大鼠体重,并行糖水偏好和强迫游泳实验,在7、14、21天做条件性恐惧实验。结果:与C组相比,CUS组和P+C组体重增加缓慢,PTSD组体重正常。CUS组于第21天出现糖水消耗比例降低,强迫游泳不动时间增加。P+C组于第14天即出现上述抑郁表现。条件性恐惧实验中,PTSD组与PTSD+CUS组僵直时间显著增加,CUS组无明显变化。结论:创伤后应激障碍的动物更易产生抑郁表现。     

造模时间对慢性不可预见性刺激致大鼠抑郁模型的影响

目的研究造模时间长短对大鼠抑郁症模型建造成功率的影响。方法将240只大鼠随机平均分为4组,各组分别给予21 d、35 d、49 d、63 d慢性温和不可预见性刺激。大鼠行为学观察指标包括旷场实验、糖水消耗实验、高架十字迷宫实验、强迫游泳实验等。结果建模成功后的抑郁大鼠其旷场的水平得分、垂直得分;高架迷宫的入开臂次数、入开臂次数比例、入开臂时间和入开臂时间比例较建模前均明显下降;糖水的消耗显著降低,旷场潜伏期时间、强迫游泳静止时间显著延长。结论随着造模时间的延长,抑郁症模型的成功率增加;延长建模时间可能会提高建模成功率,为避免资源的浪费,建议造模时间选取49 d更为恰当。     

躯体感觉Ⅱ区皮层内微刺激对猕猴回避性操作式条件反射和针刺镇痛的影响

在七只清醒、可以活动的猕猴上观察了皮层内刺激 S_Ⅱ区对外周痛阈和针刺镇痛的影响,其结果如下:(1)在73次皮层内刺激的实验中有72次引起对侧相应皮肤感受野的痛阈变化,其中54次痛阈明显升高。痛阈升高的效应在停止刺激后常持续0.5—3min。较浅层的刺激,痛阈升高比较明显;不同刺激强度引起的痛阈升高的程度也不相同。(2)一般皮层内刺激 S_Ⅱ区也可导致同侧相应皮肤感受野痛阈升高,但不如对侧痛阈升高明显。(3)皮层内刺激 S_Ⅱ区时,非感受野痛阈几乎没有任何改变。(4)S_Ⅱ区皮层内刺激可增强针刺镇痛效应。     

大鼠躯体感觉皮质即早基因c-fos表达的研究

选择性地对大鼠单根触须刺激后,通过原位杂交组织化学检测相应的躯体感觉皮质内即早基因c-fos的表达、局部定位以及与刺激强度的关系。结果表明,触须的刺激导致了相应皮质内即早基因c－fos表达增加。脑皮质第4层基因表达最明显。且基因表达量与刺激强度成正比。从脑皮质细胞组成方面证实了c-fos表达主要在皮质第4层的星形细胞;在最强的刺激后,星形细胞邻近的神经元也被标记上了。结果提示：感觉输入可影响即早基因c-fos的表达,即早基因的表达受神经元活动的调节,这种基因调节是神经元整体功能所必需的一部分。     

大鼠恐惧应激模型的建立及其视觉认知效果分析

目的构建不同程度恐惧应激大鼠模型,探究恐惧应激对LE大鼠视觉认知能力的影响。方法采用足底电击作为应激刺激,设计认知抉择实验,采集杏仁核脑区神经响应信号进行功能网络分析,评价大鼠视觉认知效果。首先,将实验大鼠分成强(S+)、弱(S)恐惧应激组与对照组(N),分别设定不同强度的足底电击刺激;然后对其进行单一图形"△"的视觉认知强化训练;最后,采用双图("△"和"十"图形)进行视觉抉择测试实验。另外结合复杂网络理论,构建恐惧应激大鼠杏仁核神经核团的视觉认知功能网络,通过平均路径长度和聚类系数表征脑功能网路的信息传递效率。结果完成视觉认知强化训练所需时间,S+组显著高于S、N组,强化训练前期S组显著高于N组,后期两组无显著性差异;认知抉择实验中,S组与N组均形成视觉认知联结,而S+组未形成视觉认知联结;脑功能网络分析中,S组与N组杏仁核神经元之间形成有效的视觉信息传递,而S+组未形成。结论恐惧应激对视觉认知造成消极影响,且随着恐惧程度的增强认知效果显著变差。     

黄酒对慢性应激大鼠肠道微生物的影响

目的 探讨黄酒对慢性应激大鼠肠道微生物的影响.方法 将45只SD大鼠制成慢性应激模型,并随机分为正常对照组、慢性应激对照组和慢性应激黄酒组.正常对照组、慢性应激对照组仅给予正常饲料喂食,慢性应激黄酒组饲料中每日添加酒精度为15.0％ (v/v)的黄酒5 mL,6周后处死大鼠,取肠道内容物做肠道乳酸菌、大肠埃希菌及真菌等微生物培养,数据采用统计学方法分析.结果 黄酒不影响大鼠的血糖变化,与正常对照组相比,慢性应激对照组乳酸菌明显减少,差异有统计学意义(P＜0.01),大肠埃希菌和真菌数量增加,差异亦有统计学意义(P＜0.05);慢性应激黄酒组乳酸菌增多,差异有统计学意义(P＜0.05),大肠埃希菌和真菌数量减少,比较差异亦有统计学意义(P＜0.05).结论 慢性应激状态下,肠道微生物发生明显的变化,适量饮用黄酒能增加肠道益生菌,减少肠道致病菌或条件致病菌,维持肠道微生态平衡,对肠道微生物有一定的调节作用.     

二甲双胍对慢性应激大鼠抑郁行为的影响

目的:观察二甲双胍对慢性不可预测性温和应激大鼠抑郁行为的影响。方法:40只雄性SD大鼠随机分为4组(n=10):对照组(CON组)、二甲双胍组(MET组)、模型组(CUMS组)、模型+二甲双胍组(CUMS+MET组),采用慢性不可预测性温和应激(CUMS)方法,用3周时间建立大鼠抑郁模型。造模完成后,两个二甲双胍组腹腔注射二甲双胍(100mg/kg),对照组和模型组注射等量的生理盐水,每天1次,连续2周。之后检测大鼠体重增长变化、糖水嗜好、强迫游泳和悬尾不动实验、旷场实验等大鼠行为学的改变,采用尼氏染色观察大鼠海马形态结构变化。结果:与对照组比较,CUMS组大鼠体重增长明显减慢(P<0.05),糖水偏爱率明显降低(P<0.05),强迫游泳和悬尾不动实验中不动时间明显延长(P<0.05),旷场实验中自发活动明显减少(P<0.05),大鼠海马的形态结构有所变化,证实CUMS抑郁模型建立成功。与CUMS组比较,二甲双胍处理后对大鼠的体重无明显影响,但能明显改善CUMS抑郁模型大鼠的糖水摄入、不动时间和自发活动(P<0.05),并能修复CUMS大鼠海马的异常形态结构变化。结论:二甲双胍对CUMS诱导的大鼠抑郁行为具有明显的改善作用,为临床糖尿病并发抑郁症的患者提供新的治疗手段。     

逍遥散对慢性束缚应激模型大鼠相关脑区CRF基因表达的影响

目的:观察慢性束缚应激大鼠相关脑区CRF mRNA(下丘脑、垂体、海马、皮层)含量变化以及逍遥散对其影响.方法:用RT-PCR和图像分析方法测定相关脑区CRF mRNA含量变化.结果:应激组较正常对照组在下丘脑CRF-1基因表达下调(P<0.01).在下丘脑逍遥散组较应激组CRF-1基因表达显著下调(P<0.01),CRF-2基因表达显著上调(P<0.01);在海马区逍遥散组CRF-2基因表达较模型组上调(P<0.05);在皮层逍遥散组CRF-1基因表达较应激组则显著上调(P<0.01).结论:逍遥散组对慢性束缚应激中枢神经肽CRF的调节位点在下丘脑、垂体、海马和皮层,充分证实逍遥散的调节靶点与下丘脑、边缘系统及皮层中枢有关.     

氟西汀对慢性不可预见应激模型大鼠海马磷脂酰乙醇胺的影响

摘要 目的：探讨氟西汀对慢性不可预见应激（Chronic Unpredictable Mild Stress,CUS）模型大鼠海马内磷脂酰乙醇胺（phosphatidylethanolamine,PE）组成的影响。方法：（1）将24只SD大鼠随机分为对照组（Sham）、模型组（CUS）和氟西汀组（Flx）。CUS组和Flx组均接受CUS造模,并且在造模后接受生理盐水（1 mL/kg）或氟西汀（10 mg/kg）腹腔注射,连续14天;Sham不进行CUS造模,但是每天接受腹腔注射生理盐水。随后处死大鼠,取海马进行脂质组学分析,比较各处理组海马总的PE和PE小分子相对丰度、不同碳链长度和含不同不饱和键PE的相对丰度差异。结果：（1）与CUS组相比,Sham组PE相对丰度明显减低,而Flx组明显增高（P<0.05）;（2）与Sham组相比,CUS组9个PE小分子相对丰度发生变化,PE（34:1e）、PE（36:1p）、PE（36:2）、PE（36:2p）、PE（36:4）、PE（38:2）、PE（38:4）和PE（40:7）共8个上调（P<0.05或0.01）,PE（34:0p）下调（P<0.05）,CUS组碳链长度为36的PE丰度上升（P<0.05）,碳链长度为38的PE丰度下降（P<0.01）,CUS组含0个不饱和键、4个不饱和键的PE丰度下调（P<0.01, P<0.05）,而1个不饱和键的PE丰度上升（P<0.05）;（3）与CUS组相比,Flx组6个PE分子相对丰度减少,包括PE（34:1e）、PE（36:2）、PE（36:4）、PE（38:1p）、PE（38:6e）和PE（40:5p）（P<0.05或0.01）,Flx组碳链长度为34的PE丰度下降（P<0.05）,碳链长度为36的PE水平升高（P<0.05）,Flx组含1个不饱和键的PE丰度下调（P<0.05）,差异具有统计学意义。结论：氟西汀可以调节CUS模型大鼠海马的PE水平。     

木豆素对慢性不可预见温和应激小鼠的抗抑郁作用

目的观察木豆素于抗抑郁方面的作用,并初步探讨其可能的作用机制。方法采用小鼠慢性不可预见温和应激模型(chronic unpredictable mild stress,CUMS),进行糖水偏好实验评价经木豆素处理的小鼠的快感缺失情况,采用酶联免疫吸附测定法测定小鼠血清皮质酮的含量,采用LC-MS/MS法检测小鼠皮层和海马中多种神经递质的含量。结果木豆素可以逆转CUMS引起的糖水偏爱指数降低和血清皮质酮水平升高。并且与正常组相比,模型组小鼠皮层和海马中相关神经递质的含量发生了显著的改变,而木豆素给药对于CUMS小鼠体内相关神经递质具有明显的调节作用。结论木豆素可能通过降低血清皮质酮水平和调节脑内神经递质来实现抗抑郁作用。     

Neonatal handling enhances contextual fear conditioning and alters corticosterone stress responses in young rats

Previous studies have indicated that neonatal handling influences development of hypothalamic-pituitary-adrenal (HPA) control of corticosterone. In addition, corticosterone influences memory consolidation processes in contextual fear conditioning. Therefore, neonatal handling may affect hippocampal-dependent memory processes present in contextual fear conditioning by influencing the development of HPA control of corticosterone. To investigate the effects of neonatal handling on early learning, rat pups were either handled (15-min removal from home cage) on the first 15 days after birth or left undisturbed in their home cage. Handled rats and nonhandled rats were fear conditioned at 18, 21, or 30 days of age and then tested at two time points--24 h following conditioning and at postnatal day 45. Subsequently, at approximately postnatal day 60, rats were exposed to restraint stress and corticosterone levels were assessed during restraint and recovery. Handled and nonhandled rats did not differ significantly in their freezing response immediately following footshock on the conditioning day. However, when tested for contextual fear conditioning at 24 h following conditioning and at postnatal day 45, handled rats showed more freezing behavior than nonhandled rats. When exposed to restraint stress, handled rats had a more rapid return of corticosterone to basal levels than nonhandled rats. These results indicate that neonatal handling enhances developmentally early memory processes involved in contextual fear conditioning and confirms previously reported effects of neonatal handling on HPA control of corticosterone.     

Recovery function of somatosensory evoked potentials in juvenile myoclonic epilepsy*

Abstract

Objective: We analysed the recovery function of somatosensory evoked potentials (SEPs) in juvenile myoclonic epilepsy (JME) patients. We hypothesized that there may be disinhibition in the recovery of SEPs at 20–100?ms intervals in JME patients.

Methods: We recorded SEPs and SEP recovery in 19 consecutive patients with JME admitted for a routine follow-up examination, and in a control group composed of 13 healthy subjects who were similar to the patient group regarding age and sex. The recovery function of SEPs was examined using paired stimuli at 30, 40, 60, and 100?ms intervals.

Results: The amplitudes of N20-P25 and P25-N33 components were higher in patients with JME. Ten patients had high-amplitude SEPs. By paired stimulation, there was inhibition of SEPs in both groups. The mean recovery percentages of N20-P25 and P25-N33 components at 30, 40, 60, and 100?ms were not different between healthy subjects and patients with JME.

Conclusions: The recovery function of SEP is normal in JME even in the presence of high-amplitude SEPs.     

The role of NCAM in auditory fear conditioning and its modulation by stress: a focus on the amygdala

Chronic stress in rodents was shown to induce structural shrinkage and functional alterations in the hippocampus that were linked to spatial memory impairments. Effects of chronic stress on the amygdala have been linked to a facilitation of fear conditioning. Although the underlying molecular mechanisms are still poorly understood, increasing evidence highlights the neural cell adhesion molecule (NCAM) as an important molecular mediator of stress‐induced structural and functional alterations. In this study, we investigated whether altered NCAM expression levels in the amygdala might be related to stress‐induced enhancement of auditory fear conditioning and anxiety‐like behavior. In adult C57BL/6J wild‐type mice, chronic unpredictable stress resulted in an isoform‐specific increase of NCAM expression (NCAM‐140 and NCAM‐180) in the amygdala, as well as enhanced auditory fear conditioning and anxiety‐like behavior. Strikingly, forebrain‐specific conditional NCAM‐deficient mice (NCAM‐floxed mice that express the cre‐recombinase under the control of the promoter of the α‐subunit of the calcium‐calmodulin‐dependent protein kinase II), whose amygdala NCAM expression levels are reduced, displayed impaired auditory fear conditioning which was not altered following chronic stress exposure. Likewise, chronic stress in these conditional NCAM‐deficient mice did not modify NCAM expression levels in the amygdala or hippocampus, while they showed enhanced anxiety‐like behavior, questioning the involvement of NCAM in this type of behavior. Together, our results strongly support the involvement of NCAM in the amygdala in the consolidation of auditory fear conditioning and highlight increased NCAM expression in the amygdala among the mechanisms whereby stress facilitates fear conditioning processes.     

慢性应激抑郁状态对大鼠外周神经内分泌因子生物节律的影响

目的：探讨慢性不可预见性应激状态下大鼠外周神经内分泌因子昼夜节律的表达特点。方法：成年雄性SD大鼠60只,随机分为模型组和对照组（n=30）,采用束缚、摇晃、鼠笼倾斜、湿垫料、冷刺激、拥挤（整夜）、断食或断水、夹尾、昼/夜颠倒等慢性不可预知性温和刺激结合孤养方式,每天暴露于2种应激原中饲养21 d,建立抑郁症模型。测定应激前后大鼠糖水偏爱、旷场行为及高架十字迷宫行为学变化。连续24 h分6个时间点（ZT1、ZT5、ZT9、ZT13、ZT17、ZT21）处死动物取血,每个时间点处死5只大鼠。放免法测定6个时间点血清促肾上腺皮质激素（ACTH）含量,ELISA法测定6个相同时间点血浆皮质酮（CORT）、褪黑素（MT）、血管活性肠肽（VIP）含量,采用单一余弦法比较2组大鼠上述各指标的节律周期、振幅、峰值相位、中值的变化特点。结果：与对照组相比,模型大鼠体重增加值明显降低（P<0.01）,各项行为学评分均显著减少（P<0.01）。慢性应激至抑郁样行为充分表达后,血浆ACTH、CORT的相位完全相反,时相大幅度提前,含量波动幅度减小,昼夜分泌节律紊乱;MT的24 h分泌节律完全丧失且整体水平下降,表达量显著降低;VIP虽仍存在24 h节律,但振幅明显降低,峰相位也延迟6 h,且表达量显著提高。结论：慢性应激抑郁状态可导致大鼠外周神经内分泌激素的近日节律非同步于SCN,表现为昼夜节律性和激素分泌量的异常。     

Prior exposure to a single stress session facilitates subsequent contextual fear conditioning in rats. Evidence for a role of corticosterone

Previous studies showed that exposure of rats to chronic restraint stress for 21 days enhances subsequent contextual fear conditioning. Since recent evidence suggest that this effect is not dependent on stress-induced neurodegenerative processes, but to elevated training-elicited glucocorticoid release in chronically stressed animals, we aimed to explore here whether a single exposure to restraint stress, which is not expected to induce neuronal damage, would also affect contextual fear conditioning. We also questioned whether post-training corticosterone levels might be associated with any potential effect of stress on fear conditioning. Adult male Wistar rats were exposed to acute restraint stress for 2 h and, two days later, trained in the contextual fear conditioning task, under training conditions involving either moderate (0.4 mA shock) or high (1 mA shock) stress levels. The results showed that acute stress enhanced conditioned freezing at both training conditions, although data from the 1 mA shock intensity experiment only approached significance. Stressed animals were shown to display higher post-training corticosterone levels. Furthermore, the facilitating effect of prior stress was not evident when animals were trained in the hippocampal-independent auditory-cued conditioning task. Therefore, these findings support the idea that stress experiences preceding exposure to new types of stressors facilitate the development of contextual fear conditioning. They also indicate that not only repeated, but also a single exposure to aversive stimulation is sufficient to facilitate context-dependent fear conditioning, and suggest that increased glucocorticoid release at training might be implicated in the mechanisms mediating the memory facilitating effects induced by prior stress experiences.     

海马NMDA受体与神经肽Y在慢性应激性抑郁发生中的作用及其关系

本文旨在探讨N-甲基-D-天冬氨酸(N-methyl-D-aspartic acid,NMDA)受体与神经肽Y(neuropeptide Y,NPY)在慢性应激抑郁发生中的作用与关系。建立慢性不可预见性温和应激(chronic unpredictable mild stress,CUMS)抑郁模型,海马单侧分别微量注射非竞争性NMDA受体拮抗剂MK-801、NPY-Y1受体阻断剂GR231118和NMDA后,利用体重测量及糖水偏爱测试、强迫游泳及敞箱实验等方法观察动物行为变化,运用免疫组织化学方法检测海马CA3区和齿状回(dentate gyrus,DG)内NPY的表达。结果显示,CUMS组大鼠表现出抑郁样行为变化,海马NPY表达显著降低;海马微量注射NMDA或NPY-Y1受体阻断剂GR231118,动物行为学表现均与CUMS组相同,注射NMDA可使NPY表达显著降低;海马微量注射MK-801能明显改善应激引起的抑郁样行为表现,并使海马NPY表达增加。联合注射GR231118与MK-801后,GR231118可以显著减弱MK-801的抗抑郁样行为的效应。以上结果表明,CUMS可能使谷氨酸(glutamic acid,Glu)过量释放,NMDA受体过度激活,抑制NPY表达,导致抑郁发生。NPY抗抑郁作用主要是通过NPY-Y1受体实现。     

The developmental effects of extremely low frequency electric fields on visual and somatosensory evoked potentials in adult rats

Abstract

The purpose of our study was to investigate the developmental effects of extremely low frequency electric fields (ELF-EFs) on visual evoked potentials (VEPs) and somatosensory-evoked potentials (SEPs) and to examine the relationship between lipid peroxidation and changes of these potentials. In this context, thiobarbituric acid reactive substances (TBARS) levels were determined as an indicator of lipid peroxidation. Wistar albino female rats were divided into four groups; Control (C), gestational (prenatal) exposure (Pr), gestational+ postnatal exposure (PP) and postnatal exposure (Po) groups. Pregnant rats of Pr and PP groups were exposed to 50?Hz electric field (EF) (12?kV/m; 1?h/day), while those of C and Po groups were placed in an inactive system during pregnancy. Following parturition, rats of PP and Po groups were exposed to ELF-EFs whereas rats of C and Pr groups were kept under the same experimental conditions without being exposed to any EF during 68 days. On postnatal day 90, rats were prepared for VEP and SEP recordings. The latencies of VEP components in all experimental groups were significantly prolonged versus C group. For SEPs, all components of PP group, P2, N2 components of Pr group and P1, P2, N2 components of Po group were delayed versus C group. As brain TBARS levels were significantly increased in Pr and Po groups, retina TBARS levels were significantly elevated in all experimental groups versus C group. In conclusion, alterations seen in evoked potentials, at least partly, could be explained by lipid peroxidation in the retina and brain.