利用生物活性小分子靶向 wnt 信号通路治疗阿尔茨海默病。

In silico pharmacology Pub Date : 2024-06-03 eCollection Date: 2024-01-01 DOI:10.1007/s40203-024-00226-z
Ankumoni Dutta, Pallab Bhattacharya, Pavitra Chutia, Anupom Borah
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摘要

阿尔茨海默病(AD)是最常见的神经退行性疾病,会破坏学习、记忆和思维能力。虽然人们对这种疾病的病理生理学了解甚少,但通过对阿尔茨海默病患者死后大脑以及动物模型的研究发现,Wnt 信号在疾病的发展过程中起着重要作用。Wnt 信号的缺失导致淀粉样 beta 肽的积累、tau 蛋白的磷酸化和突触功能障碍,这些被认为是注意力缺失症的主要病理特征。由于现有的 AD 药物只能缓解症状,而且还伴有多种副作用,因此人们正在探索生物活性化合物的治疗潜力,以了解它们在控制主要病理方面的疗效。因此,从藤黄属植物中基本分离出的一些生物活性化合物被认为是有希望治疗注意力缺失症的神经保护剂,但它们调节 Wnt 信号通路的潜力仍有待发现。考虑到其神经保护特性,本研究通过分子对接技术研究了六种小型生物活性化合物,即门黄酮、异黄酮苷、荭草苷、芹菜素、山柰酚和加西诺尔在调节 Wnt 信号通路的受体蛋白(LRP6、DKK1、WIF1 和 GSK3β)方面的效率。与已知或已报道的调制剂相比,所有生物活性化合物都能与目标蛋白有效地相互作用,其中门黄酮、荭草苷和异维黄酮苷能与所有目标蛋白(即 LRP6、DKK1、WIF1 和 GSK3β)相互作用,且结合自由能更高,相互作用次数更多,结合方式相似。因此,本研究将所研究的生物活性小分子作为治疗艾滋病的潜在候选药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Targeting of wnt signalling pathway by small bioactive molecules for the treatment of Alzheimer's disease.

Alzheimer's disease (AD) is the most occurring neurodegenerative disorder that destroys learning, memory, and thinking skills. Although the pathophysiology of the disease is least understood, the post-mortem brain of AD patients as well as animal models revealed the part of down regulated Wnt signalling in progression of the disease. The deficit in the Wnt signalling leads to the accumulation of amyloid beta peptides, phosphorylation of tau proteins, and synaptic dysfunctions, which are regarded as the major pathological features of AD. As the available drugs for AD are only able to mitigate the symptoms and are also associated with several side effects, the therapeutic potential of the bioactive compounds is being explored for their efficacies in managing the major pathologies. Consequently, a few bioactive compounds fundamentally isolated from Garcinia species are established as promising neuroprotective agents in AD, however; their potential to regulate the Wnt signalling pathway is yet to be discovered. Considering the neuroprotective properties, in the present study efficiency of six small bioactive compounds viz., amentoflavone, isovitexin, orientin, apigenin, kaempferol, and garcinol have been investigated in modulating the receptor proteins (LRP6, DKK1, WIF1 and GSK3β) of the Wnt signalling pathway by molecular docking technique. While all the bioactive compounds could efficiently interact with the target proteins, amentoflavone, orientin, and isovitexin interact with all the target proteins viz., LRP6, DKK1, WIF1, and GSK3β with higher free energy of binding, more number of interactions, and similar mode of binding in comparison to their known or reported modulators. Thus, the present study set forth the investigated small bioactive molecules as potential drug candidates in AD therapeutics.

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