REQUIMTE/Department of Chemistry and Biochemistry, University of Porto, Porto, Portugal.
Curr Med Chem. 2012;19(11):1635-45. doi: 10.2174/092986712799945058.
Alzheimer's disease (AD), a degenerative disease affecting the brain, is the single most common source of dementia in adults. The cause and the progression of AD still remains a mystery among medical experts. As a result, a cure has not yet been discovered, even after decade's worth of research that started since 1906, when the disease was first identified. Despite the efforts of the scientific community, several of the biological receptors associated with AD have not been sufficiently studied to date, limiting in turn the design of new and more potent anti-AD agents. Thus, the search for new drug candidates as inhibitors of different targets associated with AD constitutes an essential part towards the discovery of new and more efficient anti-AD therapies. The present work is focused on the role of the Ligand-Based Drug Design (LBDD) methodologies which have been applied for the elucidation of new molecular entities with high inhibitory activity against targets related with AD. Particular emphasis is given also to the current state of fragment-based ligand approaches as alternatives of the Fragment-Based Drug Discovery (FBDD) methodologies. Finally, several guidelines are offered to show how the use of fragment-based descriptors can be determinant for the design of multi-target inhibitors of proteins associated with AD.
阿尔茨海默病(AD)是一种影响大脑的退行性疾病,是成年人痴呆症的最常见病因。尽管自 1906 年首次发现该疾病以来,医学专家已经进行了长达十年的研究,但 AD 的病因和发病机制仍然是个谜。因此,尽管科学界付出了努力,但迄今为止,与 AD 相关的几种生物受体尚未得到充分研究,这反过来又限制了新型、更有效的抗 AD 药物的设计。因此,寻找新的候选药物作为与 AD 相关的不同靶点的抑制剂,是发现新的、更有效的抗 AD 疗法的重要组成部分。本工作重点介绍基于配体的药物设计(LBDD)方法的作用,这些方法已应用于阐明具有高抑制活性的新型分子实体,针对与 AD 相关的靶点。还特别强调了基于片段的配体方法作为片段药物发现(FBDD)方法的替代方法的现状。最后,提出了几条准则,以说明如何使用基于片段的描述符来设计与 AD 相关的蛋白质的多靶抑制剂。
