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Pathologically Activated Neuroprotection via Uncompetitive Blockade of N-Methyl-d-aspartate Receptors with Fast Off-rate by Novel Multifunctional Dimer Bis(propyl)-cognitin*

机译：新型多功能二聚体双（丙基）-认知素通过非竞争性阻断N-甲基-d-天冬氨酸N-甲基天门冬氨酸受体的竞争性病理激活神经保护*

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Uncompetitive N-methyl-d-aspartate (NMDA) receptor antagonists with fast off-rate (UFO) may represent promising drug candidates for various neurodegenerative disorders. In this study, we report that bis(propyl)-cognitin, a novel dimeric acetylcholinesterase inhibitor and γ-aminobutyric acid subtype A receptor antagonist, is such an antagonist of NMDA receptors. In cultured rat hippocampal neurons, we demonstrated that bis(propyl)-cognitin voltage-dependently, selectively, and moderately inhibited NMDA-activated currents. The inhibitory effects of bis(propyl)-cognitin increased with the rise in NMDA and glycine concentrations. Kinetics analysis showed that the inhibition was of fast onset and offset with an off-rate time constant of 1.9 s. Molecular docking simulations showed moderate hydrophobic interaction between bis(propyl)-cognitin and the MK-801 binding region in the ion channel pore of the NMDA receptor. Bis(propyl)-cognitin was further found to compete with [3H]MK-801 with a Ki value of 0.27 μm, and the mutation of NR1(N616R) significantly reduced its inhibitory potency. Under glutamate-mediated pathological conditions, bis(propyl)-cognitin, in contrast to bis(heptyl)-cognitin, prevented excitotoxicity with increasing effectiveness against escalating levels of glutamate and much more effectively protected against middle cerebral artery occlusion-induced brain damage than did memantine. More interestingly, under NMDA receptor-mediated physiological conditions, bis(propyl)-cognitin enhanced long-term potentiation in hippocampal slices, whereas MK-801 reduced and memantine did not alter this process. These results suggest that bis(propyl)-cognitin is a UFO antagonist of NMDA receptors with moderate affinity, which may provide a pathologically activated therapy for various neurodegenerative disorders associated with NMDA receptor dysregulation.

机译：具有快速关闭率（UFO）的非竞争性N-甲基-d-天冬氨酸（NMDA）受体拮抗剂可能代表各种神经退行性疾病的有希望的候选药物。在这项研究中，我们报告说，双（丙基）-认知素，一种新型的二聚乙酰胆碱酯酶抑制剂和γ-氨基丁酸亚型A受体拮抗剂，是NMDA受体的拮抗剂。在培养的大鼠海马神经元中，我们证明了双（丙基）认知素电压依赖性，选择性和中等抑制NMDA激活电流。双（丙基）-认知素的抑制作用随NMDA和甘氨酸浓度的增加而增加。动力学分析表明，该抑制作用起效快，抵消时效时间常数为1.9 s。分子对接模拟显示，双（丙基）-认知素与NMDA受体离子通道孔中的MK-801结合区之间存在适度的疏水相互作用。进一步发现双（丙基）-认知素与[3H] MK-801竞争，Ki值为0.27μm，并且NR1（N616R）的突变显着降低了其抑制效力。在谷氨酸介导的病理条件下，与双（庚基）-认知素相反，双（丙基）-认知素可防止兴奋性中毒，从而提高了对谷氨酸水平的提高，并且比对大脑中动脉闭塞引起的脑损伤的保护更为有效美金刚。更有趣的是，在NMDA受体介导的生理条件下，双（丙基）-认知素增强了海马切片的长期增效作用，而MK-801降低了，美金刚没有改变这一过程。这些结果表明，双（丙基）-认知素是具有中等亲和力的NMDA受体的UFO拮抗剂，可为与NMDA受体失调相关的各种神经退行性疾病提供病理激活的疗法。

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Luo, Jialie; Li, Wenming; Zhao, Yuming; Fu, Hongjun; Ma, Dik-Lung; Tang, Jing; Li, Chaoying; Peoples, Robert W.; Li, Fushun; Wang, Qinwen; Huang, Pingbo; Xia, Jun; Pang, Yuanping; Han, Yifan;
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1. Pathologically Activated Neuroprotection via Uncompetitive Blockade of N-Methyl-d-aspartate Receptors with Fast Off-rate by Novel Multifunctional Dimer Bis(propyl)-cognitin [J] . Jialie Luo, Wenming Li, Yuming Zhao, The Journal of biological chemistry . 2010,第26期

机译：通过新型多官能二聚体双（丙基）的快速离子率的N-甲基-D-天冬氨酸受体通过非竞争性封闭性的病理激活神经保护剂
2. Substantial neuroprotection against K+ deprivation-induced apoptosis in primary cerebellar granule neurons by novel dimer bis(propyl)-cognitin via the activation of VEGFR-2 signaling pathway [J] . HuS.-Q., CuiW., XuD.-P., CNS neuroscience & therapeutics . 2013,第10期

机译：新型二聚体双（丙基）-认知素通过VEGFR-2信号通路的激活，对原发性小脑颗粒神经元的K +剥夺诱导的凋亡具有实质性的神经保护作用。
3. Substantial Neuroprotection Against K + Deprivation‐Induced Apoptosis in Primary Cerebellar Granule Neurons by Novel Dimer Bis(propyl)‐Cognitin Via the Activation of VEGFR ‐2 Signaling Pathway [J] . Sheng‐Quan Hu, Wei Cui, Da‐Ping Xu, CNS neuroscience & therapeutics. . 2013,第10期

机译：新型二聚体双（丙基）-认知素通过激活VEGFR-2信号通路对原代小脑颗粒神经元的K +剥夺诱导的细胞凋亡进行实质性神经保护。
4. Molecular mechanisms underlying the neuroprotection of novel anti-Alzheimer dimers targeting pathologically activated NMDA receptors. [D] . Luo, Jialie. 2008

机译：新型抗阿尔茨海默二聚体针对病理激活的NMDA受体的神经保护的分子机制。
5. Pathologically Activated Neuroprotection via Uncompetitive Blockade of N-Methyl-d-aspartate Receptors with Fast Off-rate by Novel Multifunctional Dimer Bis(propyl)-cognitin [O] . Jialie Luo, Wenming Li, Yuming Zhao, 2010

机译：新型多功能二聚体双（丙基）-认知素通过非竞争性阻断N-甲基-d-天冬氨酸受体的竞争性与快速关闭率的病理激活的神经保护。
6. Pathologically Activated Neuroprotection via Uncompetitive Blockade of N-Methyl-D-aspartate Receptors with Fast Off-rate by Novel Multifunctional Dimer Bis(propyl)-cognitin [O] . Luo, Jialie, Li, Wenming, Zhao, Yuming, 2010

机译：新型多功能二聚体双（丙基）-认知素通过非竞争性阻断N-甲基-D-天冬氨酸受体的竞争性与快速关闭率的病理激活的神经保护。

Pathologically Activated Neuroprotection via Uncompetitive Blockade of N-Methyl-d-aspartate Receptors with Fast Off-rate by Novel Multifunctional Dimer Bis(propyl)-cognitin*

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