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首页> 外文期刊>Biological psychiatry >Dopamine D2 receptor antagonism suppresses tau aggregation and neurotoxicity
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Dopamine D2 receptor antagonism suppresses tau aggregation and neurotoxicity

机译:多巴胺D2受体拮抗作用抑制tau聚集和神经毒性

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Background: Tauopathies, including Alzheimer's disease and frontotemporal dementia, are diseases characterized by the formation of pathological tau protein aggregates in the brain and progressive neurodegeneration. Presently no effective disease-modifying treatments exist for tauopathies. Methods: To identify drugs targeting tau neurotoxicity, we have used a Caenorhabditis elegans model of tauopathy to screen a drug library containing 1120 compounds approved for human use for the ability to suppress tau-induced behavioral effects. Results: One compound, the typical antipsychotic azaperone, improved the motility of tau transgenic worms, reduced levels of insoluble tau, and was protective against neurodegeneration. We found that azaperone reduces insoluble tau in a human cell culture model of tau aggregation and that other antipsychotic drugs (flupenthixol, perphenazine, and zotepine) also ameliorate the effects of tau expression in both models. Conclusions: Reduction of dopamine signaling through the dopamine D2 receptor with the use of gene knockouts in Caenorhabditis elegans or RNA interference knockdown in human cell culture has similar protective effects against tau toxicity. These results suggest dopamine D2 receptor antagonism holds promise as a potential neuroprotective strategy for targeting tau aggregation and neurotoxicity.
机译:背景:Tauopathies,包括阿尔茨海默氏病和额颞叶性痴呆,是以脑中病理性tau蛋白聚集物的形成和进行性神经变性为特征的疾病。目前尚无有效的减轻疾病的治疗方法。方法:为了鉴定针对tau神经毒性的药物,我们使用线粒体秀丽隐杆线虫模型筛选了一个药物库,该库包含批准用于人类的1120种化合物,具有抑制tau诱导的行为效应的能力。结果:一种化合物,典型的抗精神病药氮杂哌酮,可改善tau转基因蠕虫的蠕动,降低不溶性tau的水平,并具有防止神经退行性变的作用。我们发现,氮杂哌酮可在tau聚集的人类细胞培养模型中降低不溶性tau,其他抗精神病药物(氟喷他索,奋乃静和zotepine)也可改善tau表达在两种模型中的作用。结论:利用秀丽隐杆线虫中的基因敲除或人细胞培养物中的RNA干扰敲除可减少通过多巴胺D2受体引起的多巴胺信号传导,对tau毒性具有类似的保护作用。这些结果表明,多巴胺D2受体拮抗作用有望作为针对tau聚集和神经毒性的潜在神经保护策略。

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