5,7-双羟色胺侧脑室注射对大鼠内侧前额叶皮层神经元兴奋性的影响

本研究采用在体细胞外记录的方法,探讨了双侧侧脑室注射5,7-双羟色胺(5,7-dihydroxytryptamine,5,7-DHT)损毁大鼠脑内5-羟色胺(5-hydroxytryptamine,5-HT)神经元后,内侧前额叶皮层(medial prefrontal cortex,m PFC)锥体和中间神经元兴奋性的变化。实验结果显示:5,7-DHT注射到双侧侧脑室后第2周,m PFC和中缝背核内的5-HT水平较正常组显著下降。m PFC的锥体神经元的放电频率与正常组相比明显升高,爆发式放电显著增多,而中间神经元的平均放电频率显著降低,放电形式趋向不规则活动。结果提示5-HT能递质系统对m PFC神经元活动具有重要的调节作用。     

腹腔和脑室注射促肾上腺皮质激素对大鼠不同脑区5-羟色胺含量的影响

本文应用荧光分光光度法测定脑内5-羟色胺(5-HT)含量,观察腹腔内注射(ip)或侧脑室内注射(icv)促肾上腺皮质激素(ACTH)对大鼠海马、下丘脑和中-桥脑内5-HT 含量的影响,结果如下:(1)ACTH(20.0U/kg)ip 可使海马、下丘脑和中-桥脑内5-HT 含量增多,1h达高峰,与对照组比较差异非常显著(P<0.01-0.001);ACTH ip 后3h,三脑区5-HT 含量基本恢复至对照水平。电解损毁中脑中缝核后,ACTH ip 使海马和下丘脑5-HT 含量升高的作用明显降低,摘除两侧肾上腺后,对 ACTH 增加三脑区5-HT 含量的效应没有影响。(2)ACTH(0.5U/10μl)icy 40min 后,也使三脑区5-HT 含量升高,与人工脑脊液 icv的比较,差异显著或非常显著(P<0.05-0.01);电解损毁中脑中缝核后,ACTH icv 使海马和下丘脑5-HT 含量升高的作用也显著下降。(3)ACTH ip 升高三脑区5-HT 含量的作用较 ACTH icv 的强,损毁中脑中缝核后,5-HT 含量的下降,前者却不如后者显著。上述结果提示:ACTH(ip 或 icv)之所以引起海马、下丘脑和中-桥脑5-HT 含量增多,很可能都与激活中脑中缝核有关,ACTH ip 尚可能有其它作用途径,但与肾上腺关系不大。     

褪黑素对谷氨酸钠致痫大鼠海马5-羟色胺水平的影响

目的观察褪黑素(Melatonin,MT)对谷氨酸钠(Glutamate,Glu)致痫大鼠海马5-羟色胺(5-hydroxytryptamine,5-HT)水平的影响,研究其抑制癫痫的作用机制。方法40只健康雄性SD大鼠随机分为4组(每组10只),分别为生理盐水对照组(NS组);谷氨酸钠致痫组(Glu组);褪黑素 谷氨酸钠组(MT Glu组);Luzidole 褪黑素 谷氨酸钠组(Luz MT Glu组)。观察并记录大鼠行为学及脑电图改变,用免疫组织化学方法检测大鼠海马内5-HT含量变化。结果行为学观察和EEG显示,NS组无痫样发作和痫样放电,Glu组和Luz MT Glu组痫样发作重(Ⅲ-Ⅴ级),脑电图显示频发高幅的痫样波,TM Glu组无或仅有轻微发作(0-Ⅱ级),脑电图上无或偶见散在单个微小痫样波;免疫组织化学分析结果显示,Glu组和Luz MT Glu组大鼠海马内5-HT含量与对照组比较均减少,差异性明显(P<0.05),MT Glu组较Glu组和Luz MT Glu组5-HT含量升高,差异性明显(P<0.05)。结论MT对谷氨酸钠致痫大鼠痫样发作程度、痫样放电有抑制作用,其机制之一是经由其特异性的膜受体,通过某种机制增强5-HT作用,进而发挥抑痫效应。     

姜黄素对癫痫大鼠认知功能障碍的预防作用及其可能机制

目的:探讨姜黄素(curcumin)对癫痫大鼠认知功能障碍的预防作用及其可能机制。方法:将30只成年雄性SD大鼠分为正常对照组、单纯致痫组(SE组)、姜黄素[60mg/(kg.d)]干预组(curcumin组)。采用Morris水迷宫方法检测大鼠学习记忆功能变化,并检测脑片水平的长时程增强(LTP)变化,处死大鼠后取脑组织并匀浆,测超氧化物歧化酶(SOD)、谷胱甘肽过氧化物酶(GSH-PX)、谷胱甘肽(GSH)、丙二醛(MDA)的水平。结果:(1)SE组大鼠寻找平台的潜伏期明显长于对照组,具有统计学意义(P<0.05),姜黄素组寻找平台的潜伏期相对于SE组显著缩短(P<0.05)。撤离平台后,SE组大鼠在平台所在象限的停留时间明显短于对照组(P<0.05),姜黄素治疗后大鼠在平台所在象限的停留时间较SE组显著延长(P<0.05)。(2)给予HFS刺激后各组兴奋性突出后电位(fEPSP)斜率较前明显增加,均可持续1h以上,与对照组比较SE组HFS刺激后fEPSP斜率明显减小(P<0.05),姜黄素可减轻SE所致的fEPSP斜率减小(P<0.05)。(3)SE组SOD、GSH-PX、GSH显著下降,MDA明显增高,姜黄素可逆转上述现象,有统计学意义(P<0.05)。结论:姜黄素可显著减轻癫痫持续状态所致的大鼠认知功能障碍,减轻海马区的氧化应激反应从而保护海马海马是其可能机制之一。     

维生素E 对癫痫大鼠认知功能障碍的治疗作用及其可能机制

目的:探讨维生素E(VitE)对癫痫大鼠认知功能障碍的治疗作用及其可能机制。方法:将30只成年雄性SD大鼠随机分为健康对照组、单纯致痫组(SE组)、VitE[按体重100mg/(kg.d)]干预组(VitE组)。采用Morris水迷宫实验方法检测致癫后大鼠学习记忆功能变化,同时检测脑组织匀浆中超氧化物歧化酶(SOD)、谷胱甘肽过氧化物酶(GSH-PX)、谷胱甘肽(GSH)、丙二醛(MDA)的水平。结果:(1)SE组大鼠寻找平台的潜伏期明显长于对照组,具有统计学意义(P<0.05),VitE组寻找平台的潜伏期相对于SE组显著缩短(P<0.05)。撤离平台后,SE组大鼠在平台所在象限的停留时间明显短于对照组(P<0.05),VitE治疗后大鼠在平台所在象限的停留时间较SE组显著延长(P<0.05)。(2)SE组SOD、GSH-PX、GSH显著下降,MDA明显增高,VitE干预组SOD、GSH-PX、GSH显著增高,而MDA明显下降,具有统计学意义(P<0.05)。结论:VitE可改善癫痫持续状态后大鼠认知功能,其可能机制是通过减轻海马区的氧化应激反应减轻海马区的损伤,从而实现改善认知功能。     

自杀未遂老年抑郁症患者血清5-羟色胺水平、总胆固醇、C反应蛋白及白介素-6检测的临床意义

目的:探讨自杀未遂老年抑郁症患者血清5-羟色胺(5-HT)水平、总胆固醇(TC)、C反应蛋白(CRP)及白介素-6(IL-6)检测的临床意义。方法:选取2015年5月至2018年5月我院收治的首次住院的老年抑郁症患者155例,依据入院前2周内是否曾有过自杀行为将其分为自杀未遂组(n=75)和无自杀行为组(n=80)。比较两组患者的临床指标及血清5-HT、TC、CRP及IL-6水平;分析不同病情严重程度自杀未遂老年抑郁症患者血清5-HT、TC、CRP及IL-6水平;采用Pearson相关分析血清5-HT、TC、CRP及IL-6水平与汉密尔顿抑郁量表(HAMD)评分的相关性。结果:自杀未遂组HAMD评分高于无自杀行为组(P<0.05)。自杀未遂组血清5-HT及TC水平均低于无自杀行为组(P<0.05),自杀未遂组血清CRP及IL-6水平均高于无自杀行为组(P<0.05)。与轻度组比较,中度组、重度组患者血清5-HT及TC水平均明显降低,且重度组低于中度组(P<0.05);与轻度组比较,中度组和重度组患者血清CRP及IL-6水平均明显升高,且重度组高于中度组(P<0.05)。5-HT、TC与HAMD评分呈负相关(P<0.05);CRP、IL-6与HAMD评分呈正相关(P<0.05)。结论:自杀未遂老年抑郁症患者血清5-HT、TC水平降低,CRP、IL-6水平升高,检测血清5-HT、TC、CRP及IL-6有助于评价其病情严重程度及出现自杀行为的风险。     

5,6-DHT损毁大鼠蓝斑内5-HT能神经末梢对电针镇痛的影响

在大鼠蓝斑注射5.6-DHT 以破坏其5-HT 末梢,然后观察电针镇痛效应的变化。动物分注药组和对照组,注药组在注射5.6-DHT 后7天,针刺镇痛效应比注药前显著下降。与此同时,蓝斑内的5-HT 末梢发生变性,产生逆行性荧光积累,从荧光积累的末梢走向来看,蓝斑内被5.6-DHT 损毁的5-HT 末梢主要来源于中缝背核。随着蓝斑内5-HT 末梢的变性,脑桥区5-HT 含量下降,下降率达27%P<0.01。对照组动物,蓝斑内5-HT 末梢保持正常,其镇痛效应与注药前相比也无明显改变。鉴于一般认为蓝斑核的活动削弱针刺镇痛效应,以上结果提示,在电针镇痛过程中,支配蓝斑的5-HT 神经末梢,对该核 NA 能神经元可能有抑制性影响。     

5,7-双羟色胺损毁大鼠中缝背核后底丘脑核的神经活动增强

采用玻璃微电极在体细胞外记录法,观察了5,7-双羟色胺(5,7-dihydroxytryptamine,5,7-DHT)损毁大鼠中缝背核(dorsalraphenucleus,DRN)后,底丘脑核(subthalamicnucleus,STN)神经元电活动的变化。结果发现,对照组和DRN损毁组大鼠STN神经元的放电频率分别是(6.93±6.55)Hz和(11.27±9.31)Hz,DRN损毁组大鼠的放电频率显著高于对照组(P<0.01)。在对照组大鼠,13%的神经元呈现规则放电,46%为不规则放电,41%为爆发式放电;而在DRN损毁组大鼠,具有规则、不规则和爆发式放电的神经元比例分别为9%、14%和77%,爆发式放电的STN神经元比例明显高于对照组(P<0.01)。结果显示,DRN损毁后大鼠STN神经元的放电频率增高,爆发式放电增多,提示在正常大鼠DRN抑制STN神经元的活动。     

褪黑素对谷氨酸钠致痫大鼠海马5-色胺水平的影响

目的观察褪黑素（Melatonin,MT）对谷氨酸钠（Glutamate,Glu）致痫大鼠海马5-羟色胺（5-hydroxytryptamine,5-HT）水平的影响,研究其抑制癫痫的作用机制。方法40只健康雄性SD大鼠随机分为4组（每组10只）,分别为生理盐水对照组（NS组）;谷氨酸钠致痫组（Glu组）;褪黑素＋谷氨酸钠组（MT＋Glu组）;Luzidole＋褪黑素＋谷氨酸钠组（Luz＋MT＋Glu组）。观察并记录大鼠行为学及脑电图改变,用免疫组织化学方法检测大鼠海马内5-HT含量变化。结果行为学观察和EEG显示,NS组无痫样发作和痫样放电,Glu组和Luz＋MT＋Glu组痫样发作重（Ⅲ—Ⅴ级）,脑电图显示频发高幅的痫样波,TM＋Glu组无或仅有轻微发作（0-Ⅱ级）,脑电图上无或偶见散在单个微小痫样波;免疫组织化学分析结果显示,Glu组和Luz＋MT＋Glu组大鼠海马内5-HT含量与对照组比较均减少,差异性明显（P〈0．05）,MT＋Glu组较Glu组和Luz＋MT＋Glu组5-HT含量升高,差异性明显（P〈0．05）。结论MT对谷氨酸钠致痫大鼠痫样发作程度、痫样放电有抑制作用,其机制之一是经由其特异性的膜受体,通过某种机制增强5-HT作用,进而发挥抑痫效应。     

益生菌联合常规药物对难治性癫痫患儿的疗效及对脑电图的影响CSCD

目的 探讨益生菌联合常规药物对难治性癫痫患儿的治疗效果及对患儿脑电图的影响,为该类患儿的治疗提供参考。方法 选取2020年1月至2022年5月我院收治的104例难治性癫痫患儿作为研究对象,按照随机数表法分为对照组和联合组。对照组患儿采用常规药物治疗,联合组在对照组的基础上联用益生菌治疗。对比两组患儿治疗前后癫痫发作频率、脑电图情况、炎症因子[白细胞介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)]、神经递质[γ-氨基丁酸(GABA)、5-羟色胺(5-HT)]水平及治疗后的临床疗效和用药安全性。结果 治疗前两组患儿癫痫发作频率、脑电图各频段相对功率以及IL-6、TNF-α、GABA和5-HT水平差异均无统计学意义(均P>0.05)。治疗后两组患儿癫痫发作频率、脑电图θ频段相对功率及IL-6、TNF-α水平均降低,且联合组患儿以上指标水平均低于对照组(均P<0.05)。治疗后两组患儿GABA和5-HT水平均升高,且联合组的GABA和5-HT水平高于对照组(均P<0.05)。两组患儿临床疗效分布差异有统计学意义,联合组总有效率高于对照组(94.23%vs 80.77%,P<0.05)。治疗期间两组患儿的不良反应发生率对比差异无统计学意义(P>0.05)。结论 对难治性癫痫患儿采用益生菌联合常规药物治疗能有效降低其癫痫发作频率,改善脑电图相应频段的相对功率,减轻炎症反应,抑制异常兴奋,且疗效显著,安全性高。     

The effect of intracerebroventricular 5,7-dihydroxytryptamine on morphine analgesia is time-dependent

The analgesic effect of morphine in the tail immersion test was studied in rats three and ten days after intracerebroventricular 5,7-dihydroxytryptamine (5,7-DHT) given to selectively destroy serotonergic neurons. Morphine analgesia was reduced three but not ten days after the neurotoxin. Ten days after 5,7-DHT, the inhibiting effect of metergoline, a serotonin antagonist, on morphine analgesia was still present, suggesting that functional recovery of the serotonergic system may partly explain the different results.     

Immediate and Long-Term Effects of 5,7-Dihydroxytryptamine on Rat Striatal Serotonergic Neurons Measured Using In Vivo Voltammetry

The immediate and long-term effects of the selective serotonergic neurotoxin 5,7-dihydroxytryp-tamine (5,7-DHT) on rat striatal serotonergic neurons were examined after its intracerebroventricular administration using in vivo voltammetry. Extracellular concentration of 5-hydroxyindoles increased immediately following intracerebroventricular 5,7-DHT injection (200 g in 24 l, 18 min), peaked at 1.5-2 h, and returned to normal by 4 h. 5,7-DHT diffused to the contralateral striatum in detectable amounts 9 to 12 min after the start of injection and returned to basal levels by 1.5 h. Three to 6 days after 5,7-DHT lesions, 5-hydroxytryptophan administration produced an increase in striatal 5-hydroxyindoles that was greater than that produced in pre-lesioned rats. This effect was maximal at 14 to 17 days post-lesion, and remained even after 50 days. The short-term effect of 5,7-DHT may be attributable to increased serotonin release, inhibition of uptake, or monoamine oxidase inhibition. The long-term effect of 5,7-DHT lesions may attributable to increased synthesis of serotonin or decreased reuptake in remaining serotonergic neurons.     

The short term effects of 5,7-dihydroxytryptamine on peripheral serotonin stores in Rhodnius prolixus and their long-term recovery

The serotonin neurotoxin 5,7-dihydroxytryptamine (5,7-DHT) appears to affect invertebrate systems differently from vertebrate ones. The basis for toxicity in vertebrates appears to involve the intraneuronal actions of monoamine oxidase (MAO) upon the toxin. In insects, MAO is not present in appreciable amounts. In this study, we demonstrate that in vitro 5.7-DHT competitively inhibits the uptake of [³H]serotonin by serotonergic neurohaemal areas. The apparent K_M increases from 4.9 × 10⁻⁷ to 1.7 × 10⁻⁶ M. This neurotoxin also causes a significant release of previously accumulated [³H]serotonin in nominally Ca²⁺-free saline. While 5,7-DHT does not affect the uptake of [³H]tryptophan, it reduces the subsequent synthesis of [³H]serotonin. In vivo, the tissues appear to have recovered 2 weeks after toxin treatment, as determined by immunohistochemistry. At 24 h, 1 week and 2 weeks after injection, the tissues are able to take up and release [³H]serotonin normally. 1 and 2 weeks after injection, insects ingest a normal-sized blood meal, a behaviour acutely disrupted by 5,7-DHT treatment. The results of this and other invertebrate studies suggest that 5,7-DHT does not destroy serotonergic neurons, as it does in vertebrates. 5,7-DHT may be a more useful tool to study the functions of serotonin in invertebrates as one may transiently affect serotonin stores.     

Independent effects of cholinergic and serotonergic lesions on acetylcholine and serotonin release in the neocortex of the rat

Rats received a unilateral lesion of the nucleus basalis magnocellularis (NBM) by infusion of ibotenic acid. In addition, the dorsal raphe nucleus was lesioned by infusion of 5,7-dihydroxytryptamine (5,7-DHT). The release of acetylcholine (ACh), choline, serotonin (5-HT) and 5-hydroxyindoleacetic acid (5-HIAA) was measured in the frontal neocortex by means of microdialysis. Lesions of the NBM, but not the raphe nucleus, reduced the release of ACh significantly (–47%). The release of 5-HT and 5-HIAA was reduced by raphe lesions (–44% and –79%), but not by NBM lesions. In no case did the combined lesion affect neurotransmitter release more than a single lesion. These results suggest that serotonergic projections from the dorsal raphe nucleus are not involved in tonic inhibition of ACh release in the neocortex.     

Effects of serotonin depletion on local interneurons in the developing olfactory pathway of lobsters

During embryonic life, the growth of the olfactory and accessory lobes of the lobster brain is retarded by serotonin depletion using 5,7-dihydroxytryptamine (5,7-DHT) (Benton et al., 1997). The local and projection interneurons that synapse with chemosensory cells in the olfactory lobes are potential targets of this depletion. This study documents proliferation and survival in the local interneuron cell clusters, and examines the differentiation of a prominent local interneuron, the serotonergic dorsal giant neuron (DGN), following serotonin depletion. An increase in dye coupling between the DGN and nearby cells is seen after serotonin depletion. However, morphometric analyses of individual DGNs in normal, sham-injected, and 5,7-DHT-treated embryos show that the general morphology and size of the DGNs are not significantly altered by serotonin depletion. Thus, the DGN axonal arbor occupies a greater proportion of the reduced olfactory lobes in the 5,7-DHT-treated embryos than in normal and sham-injected groups. The paired olfactory globular tract neutrophils (OGTNs), where olfactory interneurons synapse onto the DGNs, are 75% smaller in volume than the comparable region in either sham-injected or normal embryos. In vivo experiments using bromodeoxyuridine (BrdU) show that proliferation in the local interneuron soma clusters is reduced by 5,7-DHT treatment and that survival of newly proliferated local interneurons is also compromised. Our data suggest that alterations in the growth of the DGNs do not contribute to the dramatic reduction in size of the olfactory neutrophils following serotonin depletion, but that cell proliferation and survival among the local interneurons are regulated by serotonin during development. Reduced numbers of local interneurons are therefore one likely reason for the growth reduction observed after serotonin depletion.     

鞘氨醇激酶1和1-磷酸鞘氨醇受体2在癫痫大鼠海马组织中表达的变化*

目的:检测鞘氨醇激酶1 (SphK1)和1-磷酸鞘氨醇受体2 (S1PR2) 在癫痫大鼠海马中的表达,探讨SphK1和S1PR2在癫痫中的作用机制。方法:成年雄性SD大鼠108只,随机分为对照(Control)组(n=48)和癫痫(PILO)组(n=60)。癫痫组腹腔注射氯化锂(127 mg/kg),18～20 h后注射匹罗卡品,首剂量为30 mg/kg,发作＜IV级的大鼠重复注射匹罗卡品(10 mg/kg);对照组给予等剂量的生理盐水代替匹罗卡品。根据造模后观察时间和行为学改变,随机分为3个大组,6个亚组:急性期组(E6 h、E1 d、E3 d)、潜伏期组(E7 d)和慢性期组(E30 d、E56 d),每个亚组中对照大鼠和癫痫大鼠各8只。每组取4只大鼠麻醉取海马,另4只取大脑组织。运用Western blot检测SphK1、S1PR2在大鼠海马组织中的表达变化,免疫荧光检测星形胶质细胞活化增生情况及SphK1、S1PR2在星形胶质细胞中的定位表达。结果:与Control组比较,SphK1在造模后急性期(E3 d)、潜伏期(E7 d)和慢性期(E30 d、E56 d)海马中的表达均明显升高(P＜0.05或P＜0.01);S1PR2在急性期(E3 d)、潜伏期(E7 d)和慢性期(E30 d、E56 d)海马组织中的表达均明显下降(P＜0.05或P＜0.01);癫痫大鼠(E7 d)海马星形胶质细胞活化、增生明显(P＜0.05),SphK1和S1PR2在E7d的表达到位为海马星形胶质细胞中。结论:SphK1和S1PR2可能通过调控海马星形胶质细胞活化增生和影响神经元兴奋性参与了癫痫的发病。     

A topography and ultrastructural characterization ofin vivo 5,7-dihydroxytryptamine-labeled serotonin-containing neurons in the central nervous system ofAplysia californica

1. Several weeks after administration of 5,7-dihydroxytryptamine (5,7-DHT) to Aplysia, a dark pigmentation appears in serotonin-containing neurons, and this pigmentation allows visual identification of serotonergic neurons but does not appear to alter their physiology. 2. We have determined the distribution of labeled nerve cell bodies in the various ganglia of Aplysia and have characterized the pigment containing structures in both control and labeled neurons. 3. All neurons in this preparation, whether or not they utilize serotonin as a transmitter, contain pigment granules, and three types of pigment granules can be distinguished. After 5,7-DHT a new type of granule appears in serotonergic neurons, probably reflecting lysosomes that have accumulated serotonergic synaptic vesicles that contain the oxidized 5,7-DHT. 4. It remains unclear why this substance does not cause neurotoxicity in mollusks as it does in mammalian preparations.     

注射用丹参多酚酸盐联合丙戊酸钠治疗脑卒中后癫痫患者的疗效分析

目的:研究注射用丹参多酚酸盐联合丙戊酸钠对脑卒中后癫痫的临床疗效和安全性。方法:选择2016年1月～2019年4月东南大学附属中大医院江北院区神经内科住院的80例脑卒中后癫痫患者,将其随机分为两组。对照组的40例患者仅给予丙戊酸钠治疗,观察组的40例患者给予丹参多酚酸盐联合丙戊酸钠治疗。比较两组治疗后的脑电图检查结果、癫痫症状控制情况。结果:治疗后,观察组总有效率为明显高于对照组(97.50%vs. 80%,P0.05);两组的累及导联数、痫样放电、发作持续时间、发作次数较治疗前以及血清神经元特异性烯醇化酶(Neuron specific enolase,NSE)水平均较治疗前明显降低(P0.05),且观察组以上指标均明显低于对照组(P0.05)。两组的嗜睡、皮疹、头痛、感觉异常、恶心呕吐的发生率比较差异无明显统计学意义(P0.05)。结论:注射用丹参多酚酸盐联合丙戊酸钠治疗脑卒中后癫痫的疗效明显优于单用丙戊酸钠治疗,其可更有效控制癫痫症状,且安全性较高。     

Relationship between levels and uptake of serotonin and high affinity [3H]imipramine recognition sites in the rat brain

High affinity [3H]imipramine binding, endogenous levels of serotonin and noradrenaline, and serotonin uptake were determined in brain regions of rats with selective destruction of serotonergic neurons by 5,7-dihydroxytryptamine (5,7-DHT), of adrenergic neurons by 6-hydroxydopamine (6-OHDA), and of rats treated with reserpine. Neonatal treatment with 5,7-DHT resulted in a significant decrease of both serotonin levels and density (Bmax) of high affinity [3H]imipramine binding sites in the hippocampus. In contrast, an elevation of serotonin levels and an increase in Bmax of [3H]imipramine binding were noted in the pons--medulla region. No changes were observed in the noradrenaline content in either of these regions. Intracerebral 6-OHDA lesion produced a drastic suppression of noradrenaline levels in cerebral cortex but failed to alter the binding affinity (KD) or density (Bmax) of [3H]imipramine recognition sites. A single injection of reserpine (2.5 mg/kg) resulted in marked depletion of both serotonin (by 57%) and noradrenaline (by 86%) content and serotonin uptake (by 87%) in the cerebral cortex but had no significant influence of the parameters of high affinity [3H]imipramine binding in this brain region. The results suggest that high affinity [3H]imipramine binding in the brain is directly related to the integrity of serotonergic neurons but not to the magnitude of the uptake or the endogenous levels of the transmitter, and is not affected by damage to noradrenergic neurons or by low levels of noradrenaline.     

左旋组氨酸对匹罗卡品致痫大鼠癫痫发作和海马区神经细胞凋亡的影响

目的:观察左旋组氨酸(L-His)对匹罗卡品(PLO)致痫大鼠皮质脑电图及大鼠海马各区神经细胞凋亡的影响。方法:雄性SD大鼠30只,随机平均分为对照组(匹罗卡品组)、干预组(匹罗卡品+左旋组氨酸组)。各组给予相关干预处理后腹腔注射匹罗卡品建立癫痫模型,行皮质脑电图观察及海马区细胞凋亡染色观察。结果:经皮质脑电图显示,干预组潜伏期延长、痫波频率及大发作次数较对照组明显降低,差异有统计学意义(P<0.05)。凋亡染色显示,对照组的海马各区细胞在各时间点的凋亡数明显高于干预组,差异具有统计学意义(P<0.05)。结论:左旋组氨酸可以延迟匹罗卡品致痫的形成并降低点燃后癫痫发作程度,降低海马各区细胞凋亡数值,提示左旋组氨酸具有抗痫作用。