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Development of a Competition-Binding Assay to Determine Binding Affinity of Molecules to Neuromelanin via Fluorescence Spectroscopy

机译:通过荧光光谱确定分子与神经黑色素结合亲和力的竞争结合测定法的发展

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摘要

Neuromelanin, the polymeric form of dopamine which accumulates in aging neuronal tissue, is increasingly recognized as a functional and critical component of a healthy and active adult human brain. Notorious in plant and insect literature for their ability to bind and retain amines for long periods of time, catecholamine polymers known colloquially as ‘melanins’ are nevertheless curiously absent from most textbooks regarding biochemistry, neuroscience, and evolution. Recent research has brought attention to the brain pigment due to its possible role in neurodegeneration. This linkage is best illustrated by Parkinson’s disease, which is characterized by the loss of pigmented dopaminergic neurons and the ‘white brain’ pathological state. As such, the ability to determine the binding affinity of neurotoxic agents, as well as any potential specific endogenous ligands to neuromelanin are of interest and potential value. Neuromelanin has been shown to have saturable binding interactions with nicotine as monitored by a fluorimeter. This interaction provides a signal to allow for a competition-binding assay with target molecules which do not themselves produce signal. The current report establishes the viability of this competition assay toward three compounds with central relevance to Parkinson’s disease. The Kd of binding toward neuromelanin by methyl-phenyl-pyridinium ion (MPP+), dopamine, and 6-hydroxydopamine were found to be 1 mM, 0.05 mM, and 0.1 mM, respectively in the current study. In addition, we demonstrate that 6-hydroxydopamine polymerizes to form neuromelanin granules in cultured dopaminergic neurons that treated with 2,4,5-trihydroxy-l-phenylalanine. Immunohistochemical analysis using fluor-tagged anti-dopamine antibodies suggests that the incorporation of 6-hydroxydopamine (following internalization and decarboxylation analogous to levodopa and dopamine) alters the localized distribution of bound dopamine in these cells.
机译:神经黑色素是多巴胺的聚合形式,它在衰老的神经元组织中积累,被越来越多地视为健康,活跃的成年人类大脑的功能和关键组成部分。在植物和昆虫文献中臭名昭著的是其能够长时间结合和保留胺的能力,然而,有关生物化学,神经科学和进化的大多数教科书中都缺少口号为“黑色素”的儿茶酚胺聚合物。由于脑色素在神经变性中的可能作用,最近的研究引起了人们对脑色素的关注。这种联系最好用帕金森氏病来说明,该病的特征是色素多巴胺能神经元的丧失和“白脑”病理状态的丧失。这样,确定神经毒性剂的结合亲和力以及对神经黑色素的任何潜在的特定内源性配体的能力是有意义的和潜在的价值。如荧光计所监测,神经黑色素已显示与尼古丁具有饱和结合相互作用。这种相互作用提供了信号,允许与本身不产生信号的靶分子进行竞争结合测定。本报告确定了这种竞争性测定法对三种与帕金森氏病具有中心相关性的化合物的可行性。在本研究中,发现甲基-苯基-吡啶鎓离子(MPP +),多巴胺和6-羟基多巴胺与神经素结合的Kd分别为1 mM,0.05 mM和0.1 mM。另外,我们证明了6-羟基多巴胺在培养的用2,4,5-三羟基-1-苯丙氨酸处理的多巴胺能神经元中聚合形成神经黑色素颗粒。使用荧光标记的抗多巴胺抗体的免疫组织化学分析表明,6-羟基多巴胺的掺入(类似于左旋多巴和多巴胺的内在化和脱羧作用)改变了这些细胞中结合多巴胺的局部分布。

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