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The Antipsychotic D2AAK1 as a Memory Enhancer for Treatment of Mental and Neurodegenerative Diseases

机译:抗精神D2AAK1作为治疗精神和神经变性疾病的记忆增强剂

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摘要

The treatment of memory impairments associated with the central nervous system diseases remains an unmet medical need with social and economic implications. Here we show, that a multi-target ligand of aminergic G protein-coupled receptors with antipsychotic activity in vivo (D2AAK1) stimulates neuron growth and survival and promotes neuron integrity. We focused on the multilevel evaluation of the D2AAK1-related effects on neurons in terms of behavioral, cellular, molecular, and biochemical features in vivo and in vitro, such as memory-related responses, locomotor activity, tissue sections analysis, metabolic activity, proliferation level, neurons morphology, and proteins level involved in intracellular signaling pathways. In silico studies indicate that activation of calcium/calmodulin-dependent protein kinase I (CaMKI) may underline some of the observed activities of the compound. Furthermore, the compound increases hippocampal neuron proliferation via the activation of neurotrophic factors and cooperating signals responsible for cell growth and proliferation. D2AAK1 improves memory and learning processes in mice after both acute and chronic administration. D2AAK1 also causes an increase in the number of hippocampal pyramidal neurons after chronic administration. Because of its neuroprotective properties and pro-cognitive activity in behavioral studies D2AAK1 has the potential for the treatment of memory disturbances in neurodegenerative and mental diseases.
机译:与中枢神经系统疾病相关的记忆障碍的治疗仍然是社会和经济影响的未满足的医疗需求。在这里,我们展示了,体内(D2AAK1)中具有抗精神病药活性的氨基能G蛋白偶联受体的多目标配体刺激神经元生长和生存并促进神经元完整性。我们专注于在体内和体外的行为,细胞,分子和生物化学特征方面对神经元的D2Aak1相关效果的多级评估,例如记忆相关的反应,运动活性,组织切片分析,代谢活性,增殖水平,神经元形态和蛋白质水平参与细胞内信号通路。在硅研究中,表明钙/钙调蛋白依赖性蛋白激酶I(Camki)的激活可能强调了化合物的一些观察到的活性。此外,该化合物通过激活神经营养因子和负责细胞生长和增殖的配合信号增加海马神经元增殖。 D2AAK1在急性和慢性施用后改善了小鼠的记忆和学习过程。 D2Aak1还导致慢性施用后的海马金字塔神经元数增加。由于其行为研究中的神经保护性能和亲认知活性D2aak1具有治疗神经变性和精神疾病中的记忆干扰。

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