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Hybrids: a new paradigm to treat Alzheimer's disease

机译:杂种:治疗阿尔茨海默氏病的新范例

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Alzheimer's disease (AD) is a complex neurodegenerative condition with several target proteins contributing to its etiology. With 35.6 million cases worldwide documented in 2011, AD constitutes a devastating health, political, economic, and social problem for all nations. The cases are expected to increase beyond 107 million in 2050; unless an advanced therapy having a capability to delay the disease progression is developed. The curative paradigm of one-compound one-target that has been followed so far has not reached the desired mark. The research focus moved towards single molecule targeting two or more pathogenic mechanisms involved in neuronal death. Over the last few years, medicinal chemists have been paying attention to the design and synthesis of the hybrid molecules that are comprised of two pharmacophores from well-established chemical scaffolds endowed with requisite biological activities in a single entity. The hybrid-based approach has grown to be a central point in the medicinal chemistry field. Various important pharmacophores used for AD have been combined with selected biologically active molecules to get homo- and heterodimers with improved efficacy with additional supplementary actions. This review summarizes the pathogenesis of AD and various progress in the design of hybrid molecules based on the one-compound-various targets paradigm for AD therapy.
机译:阿尔茨海默氏病(AD)是一种复杂的神经退行性疾病,其中几种靶蛋白对其病因有所贡献。 2011年,AD记录了3560万例全球病例,对所有国家来说都是一个灾难性的健康,政治,经济和社会问题。预计到2050年,这些案件将增加到超过1.07亿;除非开发出具有延缓疾病进展能力的先进疗法。迄今为止一直遵循的一种复合一靶标的治疗范例尚未达到预期的目标。研究重点转向针对涉及神经元死亡的两种或多种致病机制的单分子。在过去的几年中,药物化学家一直在关注杂合分子的设计和合成,所述杂合分子由来自完善的化学支架的两个药效基团组成,所述化学支架在单个实体中具有必需的生物学活性。基于混合的方法已成为药物化学领域的中心点。各种用于AD的重要药效团已与选定的生物活性分子结合,以得到具有更高功效的同二聚体和异二聚体,并具有其他补充作用。这篇综述总结了AD的发病机理以及基于用于AD治疗的单化合物-多种靶标范式的杂交分子设计的各种进展。

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