NR2A特异性拮抗剂NVP-AAM077对大鼠海马空间学习和记忆能力的影响

目的基于经典水迷宫空间记忆行为范式,观察大鼠学习记忆前后N-甲基-D-天冬氨酸受体(N-methyl-D-aspartic acid receptor,NMDAR)2A亚单位(NR2A)变化,通过海马齿状回微量注射NVP-AAM077(NR2A拮抗剂)探讨其神经药理学作用及可能机制。方法3月龄♂SD大鼠随机分为行为学训练(Training)和未训练(Non-training)两大组,再分别分为对照和齿状回注射NVP-AAM077(NVP)组。Western blot检测齿状回的NR2A、p-eIF2α、ATF4和脑源性神经营养因子(brain-derived neurotrophic factor,BDNF)表达;向NVP组大鼠齿状回注射整合应激反应抑制剂ISRIB,观察齿状回的p-eIF2α水平、ATF4表达及空间记忆能力。结果与Non-training比较,行为学训练促进大鼠齿状回的NR2A和BDNF表达;Training-NVP大鼠齿状回的NR2A和BDNF表达明显减少,p-eIF2α和ATF4表达增加;ISRIB明显抑制ATF4表达,并翻转注射NVP引起的大鼠空间记忆损伤。结论齿状回注射NVP抑制NR2A通路激活并损害大鼠空间记忆,这种作用主要与海马整合应激反应有关。

NVP-AAM077和Ro25-6981对全脑缺血小鼠海马神经元损伤及BDNF表达的影响

目的探讨N-甲基-D-天冬氨酸受体(NMDA)亚基NR2A和NR2B特异性拮抗剂对脑缺血/再灌注后海马CA1区神经元损伤的不同影响及其可能机制。方法制作三动脉阻断(3-VO)小鼠全脑缺血模型,小鼠随机分为假手术组、脑缺血/再灌注(I/R)对照组、NVP-AAM077(NVP)干预组和Ro25-6981(Ro)干预组;应用Fluoro-JadeB(F-JB)和Nissl染色检测海马神经元变性死亡和存活情况,Western blot对脑源性神经生长因子(BDNF)蛋白表达水平进行定量分析。结果①小鼠全脑缺血12min/再灌注3d后,海马CA1区出现选择性迟发性神经元死亡,NVP干预组增加了缺血所致的海马神经元死亡(P<0.05),而Ro干预组CA1区神经元存活数量明显多于缺血/再灌注组(P<0.01);②NVP干预能明显下调缺血/再灌注所致的海马组织BDNF蛋白表达升高(P<0.01),而Ro干预能明显上调BDNF蛋白的表达(P<0.05)。结论 NMDA受体亚基NR2A和NR2B在小鼠脑缺血/再灌注损伤中具有不同的作用,其机制可能与调节BDNF表达改变有关。

An Efficient Synthesis of Selective Human NR2A Antagonist NVP-AAM077

A short and efficient synthesis of the selective human N-methyl-D-aspartate （NMDA） receptor 2A （NR2A） antagonist NVP-AAM077 is described. The target was achieved in 8 steps and in 54% overall yield from the commercially available chemical 3-methylbenzene-1,2-diamine. A NaIO4/DMF-based oxidation of the bromide to corresponding aldehyde and an addition of phosphinic acid ester to the aldimine successfully served as the key steps.

N-甲基-D-天冬氨酸受体及其亚型受体拮抗剂对抑郁大鼠的影响

目的离子型受体类药物能快速有效缓解抑郁症状,但其作用机制尚不明确。文中探讨N-甲基-D-天冬氨酸(N-methyl-D-aspartate,NMDA)受体及其亚型受体拮抗剂对强迫游泳大鼠不动时间及海马脑源性神经营养因子(brain-derivedneurotrophic factor,BDNF)表达的影响。方法雄性Wistar大鼠40只,采用随机数字表法,分为4组,每组10只。药物干预前1 d大鼠强迫游泳15 min,药物干预当天,分别腹腔注射1 ml容积等渗盐水(S组)、NVP-AAM077(NR2A受体拮抗剂)5mg/kg(NVP组)、氯胺酮(NMDA受体拮抗剂)10 mg/kg(Ket组)、Ro25-6981(NR2B受体拮抗剂)10 mg/kg(Ro组)。30 min后,记录强迫游泳大鼠不动时间,取大鼠海马组织检测BDNF。结果与S组相比,NVP组大鼠强迫游泳不动时间及海马BDNF的表达均无显著变化,而Ket组及Ro组大鼠强迫游泳时间均显著减少且海马BDNF的表达均显著增加(P<0.05)。结论氯胺酮及Ro25-6981均具有抗抑郁作用,其作用机制可能与海马BDNF的上调有关。

阻断NR2A可增强脑缺血小鼠海马神经元树突棘丢失和认知功能障碍

目的探讨N-甲基-D-天门冬氨酸受体(N-methyl-D-aspartate receptor,NMDAR or NR)亚基NR2A在脑缺血再灌注引起的海马CA1区神经元树突棘丢失和认知功能障碍中的作用。方法制作三动脉阻断(3-VO)GFP转基因小鼠全脑缺血模型,小鼠随机分为假手术组、脑缺血再灌注(I/R)组和NVP-AAM077(NVP)干预组;应用跳台试验测试小鼠学习记忆能力,激光共聚焦和Neurolucida软件分析检测海马CA1区神经元形态及树突棘的变化。结果学习记忆能力测试发现,I/R组明显差于sham组(P<0.05),NVP干预组差于sham组和I/R组(P<0.05);I/R组CA1区神经元树突棘的数量明显少于假手术组(P<0.01),NVP干预能进一步增加缺血/再灌注所致的CA1区神经元树突棘的丢失(P<0.05)。结论 NMDA受体亚基NR2A在小鼠脑缺血再灌注所致树突棘丢失和脑认知功能损害中具有重要作用。

Synergistic Suppression of Cortical Spreading Depression under NR2A and NR2B Inhibition

Cortical spreading depression (CSD) is a transient synaptic excitation, followed by depression, which can propagate slowly across cortex, subcortex and retina. CSD is implicated in migraine with aura and may lead to migraine pain. CSD can be suppressed by inhibition of both NR2A and NR2B containing N-methyl-D-aspartic acid (NMDA) receptors. However, whether there is a synergistic effect of co-inhibition of NR2A and NR2B containing receptors on CSD remains unknown. In this study, an efficient in vitro model of migraine with intrinsic optical imaging approach was applied to address this role of co-activation of both NR2A and NR2B in CSD. The results showed that co-application of NVP-AAM077, a drug selectively targeting for NR2A and Ro 25-6981, a drug selectively targeting for NR2B containing receptors, showed synergistic inhibitory effects on propagation rate and the magnitude of CSD in a concentration dependent manner in chick retina. Inhibition of CSD propagation was also observed by a clinical acceptable drug that antagonizes both NR2A and NR2B containing receptors, memantine, at 10 μM. These data suggest that combinational use of antagonists selectively targeting NR2A and NR2B containing receptors could be a useful strategy for preventative treatment of migraine with improved efficacy with potential alleviated side effects.

OP-07的更新换代产品——OP-77运算放大器

ＯＰ－７７运算放大器是ＯＰ－０７的更新换代产品。本文不仅对ＯＰ－７７与ＯＰ－０７运算放大器的基本性能指标进行了对比，而且还指出了它们的共同点和差异。

HOE077对胰岛细胞微囊外纤维化反应及其活力的影响

目的 研究抗肝纤维化药物HOE 0 77对胰岛微囊外纤维化反应及细胞活力的影响。方法 猪胰岛分离后包裹在海藻酸钡微囊内 ,移植于Balb/c小鼠肝内。术后HOE 0 77通过溶解于饮用水中给药 ,对照组饮水中不含HOE 0 77。 1个月后处死动物 ,病理检查观察包囊外的纤维化反应程度 ,评价囊内细胞的存活情况。结果 对照组显示了明显的纤维化反应 ,纤维包裹层厚度平均为(6 2 .12± 3.84) μm ,细胞活力为 (15 .16± 2 .32 ) % ;而HOE 0 77治疗组纤维包裹厚度为 (4 1.44±2 .45 ) μm ,活力为 (2 3 .0 8± 2 .45 ) %。统计学分析表明 ,两组在囊外纤维包裹层的厚度及细胞活力上差异均有显著性 (P <0 .0 0 0 1和P <0 .0 1)。结论 抗肝纤维化药物HOE 0

和谐型机车电子制动阀(EBV)077代码故障分析及对策

对和谐型机车电子制动阀(EBV)077代码故障产生的原因进行了分析,并提出了相应的对策措施。