The impact of chelating compounds on Cu2+, Fe2+/3+, and Zn2+ ions in Alzheimer's disease treatment

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Tomasz Mazur, Magdalena Malik, Dariusz C. Bieńko
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Abstract

Alzheimer's disease (AD) is a neurodegenerative disorder characterized by the accumulation of amyloid – β extracellular plaques and tau interfibrillar tangles, leading to memory loss, cognitive decline, and behavioral changes. With dementia posing a growing global health concern, there is an urgent need for comprehensive strategies to address its challenges. The economic burden of dementia is projected to rise significantly, emphasizing the necessity for collaborative efforts in research and healthcare. In the United States alone, millions are affected by AD, with prevalence increasing with age and even affecting younger individuals. The complexity of AD involves intricate biological processes, including the aggregation of amyloid beta, oxidative stress, and metal ion dysregulation. Metal ions, particularly those from copper, iron, and zinc, play pivotal roles in AD pathology, influencing Aβ deposition and tau protein accumulation. Current treatments offer symptomatic relief but do not address the underlying disease mechanisms. This paper explores the potential of various chelating compounds to target metal ions involved in AD pathology. N-acylhydrazones, morpholine, chrysin, quinoline, oxindole, cyclam, catechol-based, and quinazolinone-based derivatives show promising chelation activity and therapeutic effects.

Metal chelation therapy offers a targeted approach to AD treatment by addressing the core pathology. By selectively binding to metal ions implicated in disease progression, chelators may minimize side effects associated with broad-spectrum treatments. Additionally, chelators may offer neuroprotective effects beyond metal binding, further enhancing their therapeutic potential. Overall, metal chelation therapy presents a promising strategy in combating AD, with the potential to significantly impact disease progression and improve patient outcomes.

Abstract Image

螯合化合物对阿尔茨海默病治疗中 Cu2+、Fe2+/3+ 和 Zn2+ 离子的影响
阿尔茨海默病(AD)是一种神经退行性疾病,以淀粉样蛋白-β细胞外斑块和 tau 纤维间缠结的积累为特征,导致记忆力减退、认知能力下降和行为改变。随着痴呆症成为日益严重的全球健康问题,迫切需要制定综合战略来应对其挑战。据预测,痴呆症造成的经济负担将大幅增加,这就强调了在研究和医疗保健领域开展合作的必要性。仅在美国,就有数百万人受到老年痴呆症的影响,发病率随着年龄的增长而增加,甚至影响到年轻人。注意力缺失症的复杂性涉及错综复杂的生物过程,包括淀粉样蛋白 beta 的聚集、氧化应激和金属离子失调。金属离子,尤其是铜、铁和锌离子,在 AD 病理学中起着关键作用,影响着 Aβ 的沉积和 tau 蛋白的积累。目前的治疗方法可缓解症状,但无法解决潜在的疾病机制。本文探讨了各种螯合化合物靶向参与注意力缺失症病理的金属离子的潜力。N-酰肼、吗啉、金丝桃素、喹啉、吲哚、环胺、儿茶酚基和喹唑啉酮基衍生物显示出良好的螯合活性和治疗效果。螯合剂通过选择性地结合与疾病进展有关联的金属离子,可以最大限度地减少广谱疗法的副作用。此外,螯合剂还能提供金属结合之外的神经保护作用,从而进一步提高其治疗潜力。总之,金属螯合疗法是一种很有前景的抗击注意力缺失症的策略,有可能显著影响疾病的进展并改善患者的预后。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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