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一种新型的优先结合铁(II)的多巴胺激动剂螯合剂,作为帕金森病潜在的对症和神经保护治疗剂。

A Novel Iron(II) Preferring Dopamine Agonist Chelator as Potential Symptomatic and Neuroprotective Therapeutic Agent for Parkinson's Disease.

作者信息

Das Banibrata, Kandegedara Ashoka, Xu Liping, Antonio Tamara, Stemmler Timothy, Reith Maarten E A, Dutta Aloke K

机构信息

Department of Pharmaceutical Sciences, Wayne State University , Detroit, Michigan 48202, United States.

Department of Psychiatry, New York University , New York, New York 10016, United States.

出版信息

ACS Chem Neurosci. 2017 Apr 19;8(4):723-730. doi: 10.1021/acschemneuro.6b00356. Epub 2017 Jan 27.

Abstract

Parkinson's disease (PD) is a progressive neurodegenerative disorder, and development of disease-modifying treatment is still an unmet medical need. Considering the implication of free iron(II) in PD, we report here the design and characterization of a novel hybrid iron chelator, (-)-12 (D-607) as a multitarget-directed ligand against PD. Binding and functional assays at dopamine D/D receptors indicate potent agonist activity of (-)-12. The molecule displayed an efficient preferential iron(II) chelation properties along with potent in vivo activity in a reserpinized PD animal model. The compound also rescued PC12 cells from toxicity induced by iron delivered intracellularly in a dose-dependent manner. However, Fe selective dopamine agonist 1 and a well-known antiparkinsonian drug pramipexole produced little to no neuroprotection effect under the same experimental condition. These observations strongly suggest that (-)-12 should be a promising multifunctional lead molecule for a viable symptomatic and disease modifying therapy of PD.

摘要

帕金森病(PD)是一种进行性神经退行性疾病,开发疾病修饰疗法仍然是未满足的医学需求。考虑到游离亚铁在帕金森病中的作用,我们在此报告一种新型杂化铁螯合剂(-)-12(D-607)作为针对帕金森病的多靶点导向配体的设计与表征。对多巴胺D/D受体的结合和功能测定表明(-)-12具有强效激动剂活性。该分子显示出高效的优先亚铁螯合特性以及在利血平化帕金森病动物模型中的强效体内活性。该化合物还以剂量依赖性方式挽救PC12细胞免受细胞内递送的铁诱导的毒性。然而,在相同实验条件下,铁选择性多巴胺激动剂1和著名的抗帕金森病药物普拉克索几乎没有产生神经保护作用。这些观察结果强烈表明,(-)-12应该是一种有前景的多功能先导分子,用于可行的帕金森病症状性和疾病修饰治疗。

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