低剂量伽玛刀照射对致大鼠皮质及海马神经元c-fos和nNOS表达的影响

目的 通过观察低剂量伽玛刀照射对致痫大鼠大脑皮质及海马神经元c—fos和脑型一氧化氮合酶（nNOS）表达的影响，探讨伽玛刀治疗癫痫的作用机制。方法将44只青霉素致痫大鼠模型等分为实验组和实验对照组大鼠各22只，另取4只正常大鼠作为正常对照组。实验组行伽玛刀照射（周边剂量12Gy）后，应用免疫组化方法，观察大脑皮质及海马神经元c-fos和nNOS表达的变化。结果无论是皮质还是海马，c—fos和nNOS在实验组与实验对照组动物之间，表达均有明显的差别，实验组表达明显少于实验对照组，而后者呈现双高峰现象。结论c—fos和nNOS在伽玛刀治疗癫痫的机制中发挥了重要作用。     

小剂量伽玛刀照射对致癎大鼠脑神经元nNOS表达的影响

目的 通过观察低剂量伽玛刀照射对致痫大鼠大脑皮质及海马神经元nNOS表达的影响，初步探讨伽玛刀治疗癫痫的作用机制。方法 将44只青霉素致痫大鼠模型等分为实验组和实验对照组，对实验组进行伽玛刀照射（周边剂量12Gy），应用免疫组化方法检测两组大脑皮质及海马神经元nNOS表达的变化。结果 nNOS在两组动物的皮质和海马表达均有显著性差别．实验组显著性低于实验对照组；实验对照组表达呈双高峰现象。结论 nNOS在伽玛刀治疗癫痫的机制中具有重要作用。     

低剂量伽玛刀对致痫大鼠皮层及海马神经元Fos表达的影响

目的通过观察低剂量伽玛刀照射对致痫大鼠大脑皮质及海马神经元cfos表达的影响,初步探讨伽玛刀治疗癫痫的作用机制,为临床治疗提供理论依据。方法以青霉素致痫模型为对象,应用免疫组化方法,检测低剂量伽玛刀照射(周边剂量12Gy)后,大脑皮质及海马神经元cfos表达的变化。实验组和对照组大鼠各22只,正常对照组大鼠4只。结果无论是皮层还是海马,伽玛刀照射后cfos在实验组动物和对照组动物中,表达均有明显的差别,并随时间呈现一定的规律性。结论cfos在伽玛刀治疗癫痫的机理中发挥重要作用。     

低剂量伽玛刀照射癫癎大鼠脑神经元的超微结构研究

目的探索伽玛刀治疗原发性癫的细胞学机理。方法建立大鼠皮质青霉素局灶性癫癎模型,将SD大鼠随机分为实验组、实验对照组和对照组。照射周边剂量12 Gy, 等剂量曲线为50%。分别于0.5 h~2个月后取靶区皮质及海马标本制备光镜、常规透射电镜样品。结果癫癎模型鼠可见较多凋亡神经元,而癫癎模型鼠经低剂量伽玛刀照射后同时程的神经元改变较轻微,凋亡细胞少见。结论凋亡参与了青霉素致癫癎发作后海马神经元的死亡过程,低剂量伽玛刀照射对抑制神经元的死亡过程有重要作用。     

托吡酯对戊四氮致癫癎大鼠海马AQP4表达水平的影响

目的探讨托吡酯对戊四氮致癫癎大鼠海马AQP4表达水平的影响。方法将30只Wistar大鼠随机分为戊四氮致癫癎组、托吡酯干预组和正常对照组，每组各10只；癫癎模型点燃后在不同时相点灌注取材，通过HE染色观察大鼠海马神经元的变化，并应用免疫组化法检测大鼠海马AQP4表达水平。结果HE染色显示托吡酯干预组神经元变性和坏死较戊四氮致癫癎组明显减轻；免疫组化显示戊四氮致癫癎组在致癫癎后12hAQP4的表达显著增强，致癫癎后24h达高峰，托吡酯干预组在致癫癎后12h～36h各时相点AQP4表达水平均分别低于戊四氮致癫癎组相应时间点（P〈0．05）。结论托吡酯通过下调大鼠海马AQP4的表达可能参与了对大鼠海马神经元的保护过程。     

喹啉对癫(癎)大鼠海马神经元连接蛋白36表达的影响

目的:探讨喹啉对癫癎大鼠海马神经元连接蛋白36(Cx36)表达的影响.方法:64只SD大鼠随机分为正常对照组、癫癎模型组、地西洋治疗组和喹治疗组,每组16只大鼠.采用氯化锂-匹罗卡品诱导制作癫癎大鼠模型,地西泮治疗组子以1mg/kg地西泮治疗,喹啉治疗组予以60mg/kg喹啉治疗.术后分别采用Racine评分和脑电图检查判断癫癎发作情况.分别用免疫荧光染色法、Western blot法检测各组大鼠术后2h、4h时海马神经元Cx36的表达.结果:与正常对照组比较,癫癎模型组和地西泮治疗组大鼠术后2h、4h时海马神经元Cx36表达水平显著升高(均P<0.01).癫癎模型组和地西泮治疗组大鼠术后2h、4h时海马神经元Cx36表达水平比较差异无统计学意义.与癫癎模型组及地西泮治疗组比较,喹啉治疗组大鼠术后2h、4h时海马神经元Cx36表达水平显著降低(均P<0.01).结论:癫癎大鼠海马神经元Cx36表达水平升高,喹啉能抑制这一变化.     

伽玛刀低剂量照射对致疒间大鼠海马中氨基酸递质的影响

目的观察伽玛刀低剂量照射对致疒间大鼠海马中谷氨酸(Glu)、γ-氨基丁酸(GABA)的影响,探讨伽玛刀治疗癫疒间的作用机制。方法将50只锂-匹罗卡品致疒间大鼠随机分为照射组和非照射组,各25只,另取正常大鼠25只(腹腔注射生理盐水)作为对照组。照射组大鼠进行伽玛刀低剂量照射(周边剂量20Gy),对照组和非照射组大鼠不进行伽玛刀照射。用高效液相色谱-质谱-质谱(HPLC-MS-MS)分析法检测各组大鼠海马Glu、GABA的含量。结果伽玛刀照射2周后,照射组和非照射组大鼠海马中Glu含量均高于对照组,照射组GLu含量低于非照射组,差异具有统计学意义(P0.05);照射组和非照射组GABA含量均低于对照组,照射组GABA含量高于非照射组,差异具有统计学意义(P0.05)。结论伽玛刀低剂量照射通过调节海马中Glu与GABA的平衡,以达到抗癫疒间的作用。     

氟桂利嗪对青霉素致痈效应和海马神经元单位放电的影响

目的：探讨Ca^2＋拮抗剂氟桂利嗪对青霉素致效应和海马神经元单位放电的影响.方法：Wistar大鼠随机分成3组.正常对照组;癫癎模型组：用青霉素钠按6 000 000 U·kg^-1腹腔注射;癫癎预处理组：造模前用盐酸氟桂利嗪 20 mg·kg^-1每隔12 h灌胃,共2次,于第2次给药2 h后制作模型.观察癫癎发作并记录海马神经元单位放电.结果： ①正常对照组大鼠共记录到24个单位海马神经元放电;②癫癎模型组共记录到78个单位海马神经元放电,癫癎发作程度强,发作频率高;③癫癎预处理组共记录到47个单位海马神经元放电,癫癎发作程度减轻,发作频率减少.结论：氟桂利嗪可抑制青霉素致效应,减少海马神经元的单位放电.     

颞叶癫大鼠海马轴突导向分子Sema3F及其受体Np2表达的变化

目的 研究颞叶癫(癎)大鼠海马轴突导向分子Sema3F及其受体Np2表达的变化.方法 给SD大鼠腹腔注射匹罗卡品、氯化锂制作颞叶癫(癎)模型.用免疫组化法和原位杂交技术对致(癎)后不同时间点大鼠海马CA1区、CA3区、齿状回的Sema3F mRNA、Np2 mRNA和蛋白表达进行检测,并与正常对照组比较.结果 颞叶癫(癎)大鼠致(癎)后7 d、15 d,海马CA1区、CA3区Sema3F mRNA、Np2 mRNA和蛋白的表达明显低于正常对照组(P＜0.05～0.01), 致(癎)后30 d、60 d表达与正常对照组差异无统计学意义;而齿状回Sema3F mRNA、Np2 mRNA和蛋白的表达与正常对照组的差异无统计学意义.结论 颞叶癫(癎)大鼠海马CA1区、CA3区Sema3F、Np2表达在致(癎)后早期明显下调,而在慢性期恢复正常.     

雌激素致癎作用部位的研究

目的了解雌激素在癫癎大鼠中枢神经系统的作用部位.方法利用海人酸致癎和6-氟二乙酯致癎的两种不同机制的癫癎模型(单纯致癎组),应用免疫组化法检测单纯致癎及给予雌激素后再致癎大鼠海马、大脑皮质、纹状体的FOS表达.结果两种模型单纯致癎组海马、皮质、纹状体FOS表达较正常组显著增高(均P＜0.01).给予雌二醇(E2)后再致癎,海人酸模型中海马、皮质FOS表达较单纯致癎组增加(P＜0.01,P＜0.05);而6-氟二乙酯模型中无变化.结论在两种不同致癎机制的癫癎模型中,雌二醇对鼠脑FOS表达的影响不同.     

The neuroendocrinology of stress and the pathophysiology and therapy of depression and anxiety

Clinical and preclinical studies have gathered substantial evidence that stress response alterations play a major role in the development of major depression, panic disorder, and post-traumatic stress disorder. The stress response, the hypothalamic pituitary adrenocortical (HPA) system and its modulation by corticotropin-releasing hormones (CRH),corticosteroids,and their receptors, and the roles of natriuretic peptides and neuroactive steroids are described. We review the role of the HPA system in major depression, panic disorder, and post-traumatic stress disorder and its possible relevance for treatment. Impaired glucocorticoid receptor function in major depression is associated with an excessive release of neurohormones such as CRH, to which a number of signs and symptoms characteristic of depression can be ascribed. In panic disorder, a role of central CRH in panic attacks has been suggested. Atrial natriuretic peptide (ANP) is causally involved in sodium lactate-induced panic attacks. Furthermore, preclinical and clinical data on its anxiolytic activity suggest that nonpeptidergic ANP receptor ligands may be potentially useful in the treatment of anxiety disorders. Post-traumatic stress disorder is characterized by a peripheral hyporesponsive HPA system and elevated CRH concentrations in the CSF. This dissociation is probably related to an increased risk of this disorder. We further review recent data that describe an important role of GABA(A)-receptor modulatory,3 alpha-reduced neuroactive steroids in major depression, anxiety, and its treatment. Antidepressants are effective in both depression and anxiety disorders and have major effects on the HPA system,especially on glucocorticoid and mineralocorticoid receptors. Normalization of HPA system abnormalities is a strong predictor of the clinical course, at least in major depression and panic disorder. Currently,CRH-R1 or glucocorticoid receptor antagonists and ANP receptor agonists are being studied and may provide future treatment options more closely related to the pathophysiology of these disorders.     

Polymorphisms of DRD4 and DRD3 and risk of avoidant and obsessive personality traits and disorders

We investigated whether polymorphisms of the dopamine D4 receptor (DRD4) and polymorphisms of the dopamine D3 receptor (DRD3) were associated with personality disorder symptomatology rather than with personality traits such as novelty seeking. DNA was obtained from 145 depressed patients in a clinical trial. These patients were assessed for the presence of personality disorder symptoms and disorders. The 2-repeat allele of the DRD4 exon III polymorphism was associated with increased rates of avoidant and obsessive personality disorder symptomatology. The T,T genotype of the DRD4 -521 C>T polymorphism was also associated with increased rates of avoidant and obsessive personality disorder symptomatology. The Gly9,Gly9 genotype of the DRD3 Ser9Gly polymorphism was associated with increased rates of obsessive personality disorder symptomatology. None of these three polymorphisms were associated with novelty seeking or other temperament traits on the Temperament and Character Inventory. Our results suggest that genetic polymorphisms of DRD4 and DRD3 may well be associated with personality traits, and that conflicting findings to date may arise from the problem of phenotype definition.     

沙盘游戏疗法在地中海贫血患儿心理干预中的应用

本文目的是对沙盘游戏疗法在地中海贫血患儿心理干预中的应用进行综述,以期为地中海贫血患儿的心理康复提供参考。地中海贫血是以珠蛋白生成障碍为主要特征的遗传性疾病,由于长期输血治疗,患儿存在较多的心理和行为问题。沙盘游戏疗法作为一种有效、实用的儿童心理治疗方法,对提高地中海贫血患儿的康复效果、改善生存质量有重要的临床意义。     

癫痫共病抑郁的机制及临床诊疗

本文目的是探讨癫痫共病抑郁的可能机制及临床诊疗。癫痫是一种常见的、慢性的、致残性的神经疾病,癫痫患者生活质量下降,存在明显的负性情绪,常伴发各种精神疾病。癫痫与抑郁具有共同的神经生物学基础,可能存在共同的发病机制。本文从癫痫共病抑郁的发病机制、临床诊断及治疗方面予以总结归纳。     

Efficacy and Effectiveness of Child and Adolescent Psychotherapy and Pharmacotherapy

Decades of intervention research have produced a rich body of evidence on the effects of psychotherapies and pharmacotherapies with children and adolescents. Here we summarize and critique that evidence. We review findings bearing on the efficacy of psychosocial treatments and medications under controlled experimental conditions. We also report evidence, where available, on the effectiveness of both classes of treatment with clinically referred youth treated in real-world clinical contexts. In general, the large body of evidence on efficacy contrasts sharply with the small base of evidence on effectiveness. Addressing this gap through an enriched research agenda could contribute importantly to linking scientific inquiry and clinical practice—to the benefit of both ventures. This is one element of a multifaceted agenda for future research and for synthesis of research, which will require the interplay of multiple disciplines related to child and adolescent mental health.     

Seclusion and restraint and prediction of violence

The authors studied the use of seclusion and restraint on an inpatient unit in a state psychiatric hospital. Of 69 randomly selected inpatients, 51% experienced seclusion or restraint at least once. More psychotic than nonpsychotic patients required seclusion or restraint. However, neither psychosis/nonpsychosis nor voluntary/involuntary admission status predicted the likelihood of violent threats or actions. Patients experiencing seclusion and restraint showed a nonsignificant trend toward longer mean length of stay in the hospital. The frequency of patient behavior leading to seclusion or restraint appeared to be directly related to the stimulation caused by the presence of many staff members and other patients.     

Comparison of trigeminal and spinal modulation of pain and nociception

Modulation of pain and nociception by noxious counterstimulation, also called "diffuse noxious inhibitory controls" or DNIC-like effect, is often used in studies of pain disorders. It can be elicited in the trigeminal and spinal innervation areas, but no study has previously compared effects in both innervation areas. Therefore, we performed a study comparing DNIC-like effects on the nociceptive flexion reflex (NFR) and the nociceptive blink reflex as well as the respective pain sensations. In 50 healthy volunteers, the blink reflex elicited with a concentric electrode and the NFR were recorded before and after immersion of the contralateral hand in cold water. Responses were recorded as the subjective pain sensation and the reflex size. The cold water immersion of the contralateral hand elicited a reduction of both subjective pain sensation and reflex amplitude following the stimulation of both reflexes. However, there were no strong correlations between the individual reductions of both subjective pain sensation and reflex amplitude for both reflexes, and neither when results of the two reflexes were compared with each other. The dissociation between DNIC-like effects on pain and on nociception, which had been found previously already for the NFR, implies that both effects need to be studied separately.