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The art of building multifunctional metal-binding agents from basic molecular scaffolds for the potential application in neurodegenerative diseases

机译:由基本分子支架构建多功能金属结合剂的技术在神经退行性疾病中的潜在应用

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摘要

Metal-ion homeostasis in the brain is critical for many physiological functions, particularly in the central nervous system where metals are essential in complex signaling pathways. Most common neurological diseases such as Alzheimer's (AD), Parkinson's (PD) and prion diseases, despite having distinct etio-logical bases, share similarities associated with metalloprotein misfolding and aggregation. In the last few years, several studies have provided evidence that abnormal concentrations of Cu(II), Zn(II) and/or Fe(III) specifically impair protein deposition and/or cause oxidative damage. This apparently critical role played by metal imbalance makes chelation therapy an attractive and challenging strategy to alleviate the development and progression of neurological disorders. Due to the multiple factors closely involved in the pathogenesis of these diseases, the classic drug discovery paradigm of "one molecule, one target-is limited in its ability to combat such complex diseases. Therefore, significant effort has been devoted to designing multifunctional metal-chelators aiming at multiple targets that must be addressed in these neurodegenerative diseases. In this review, the state-of-the-art in this latest strategy for designing metal-ion chelators as potential therapeutic agents in neurodegenerative diseases will be discussed, with special emphasis on AD and additional coverage of PD and prion diseases.
机译:大脑中的金属离子稳态对于许多生理功能至关重要,特别是在中枢神经系统中,金属是复杂信号通路必不可少的。尽管具有不同的病因基础,但最常见的神经系统疾病,例如阿尔茨海默氏病(AD),帕金森氏症(PD)和病毒疾病,都具有与金属蛋白错误折叠和聚集相关的相似性。在过去的几年中,一些研究提供了证据表明异常浓度的Cu(II),Zn(II)和/或Fe(III)特别损害蛋白质沉积和/或引起氧化损伤。金属不平衡发挥的这一明显的关键作用使螯合疗法成为缓解神经系统疾病发展和进程的有吸引力且具有挑战性的策略。由于与这些疾病的发病机理密切相关的多种因素,“一种分子,一个靶标”的经典药物发现范式在抵抗此类复杂疾病的能力方面受到限制。因此,人们致力于设计多功能金属-针对这些神经退行性疾病中必须解决的多个目标的螯合剂。在本综述中,将讨论设计金属离子螯合剂作为神经退行性疾病的潜在治疗剂的最新策略中的最新技术。关于AD以及PD和病毒疾病的额外覆盖。

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