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载胰岛素的胍基修饰杯芳烃与环糊精共组装体对阿尔茨海默病的多靶点治疗

Multi Targeted Therapy for Alzheimer's Disease by Guanidinium-Modified Calixarene and Cyclodextrin Co-Assembly Loaded with Insulin.

作者信息

Zhang Qi-Yue, Wang Qiang, Fu Jing-Xuan, Xu Xin-Xin, Guo Dong-Sheng, Pan Yu-Chen, Zhang Tao, Wang Hui

机构信息

Key Laboratory of Molecular Biophysics, Hebei Province, Institute of Biophysics, School of Health Sciences and Biomedical Engineering, Hebei University of Technology, Tianjin 300401, P. R. China.

College of Life Sciences and Key Laboratory of Bioactive Materials Ministry of Education, Nankai University, Tianjin 300071, P. R. China.

出版信息

ACS Nano. 2024 Dec 3;18(48):33032-33041. doi: 10.1021/acsnano.4c05693. Epub 2024 Nov 5.

Abstract

Amyloid-β (Aβ) is considered a primary therapeutic target for Alzheimer's disease (AD). However, just eliminating Aβ in patients with AD has exhibited restricted clinical efficacy, possibly failing to address the metabolic abnormalities caused by AD, such as insulin resistance. To address this concern, our research has employed two types of macrocyclic amphiphiles, guanidinium-modified calixarene and cyclodextrin coassembly (GCD), as delivery systems for insulin. This approach aimed to tackle the metabolic dysregulation characteristic of AD in an innovative manner by exploring beyond the conventional strategy of Aβ removal. As a result, GCD and insulin coassembly could effectively improve plaque deposition and insulin resistance. The coassembly could also reduce abnormal neuronal apoptosis and synaptic damage and improve cognitive impairment in 5xFAD mice. Therefore, the GCD and insulin coassembly shows promise as a viable therapeutic option for AD.

摘要

淀粉样蛋白-β(Aβ)被认为是阿尔茨海默病(AD)的主要治疗靶点。然而,仅仅在AD患者中清除Aβ已显示出有限的临床疗效,可能无法解决由AD引起的代谢异常,如胰岛素抵抗。为了解决这一问题,我们的研究采用了两种大环两亲物,即胍基修饰的杯芳烃和环糊精共组装体(GCD),作为胰岛素的递送系统。这种方法旨在通过超越传统的Aβ清除策略,以创新的方式解决AD的代谢失调特征。结果,GCD与胰岛素的共组装体能够有效改善斑块沉积和胰岛素抵抗。该共组装体还可以减少异常的神经元凋亡和突触损伤,并改善5xFAD小鼠的认知障碍。因此,GCD与胰岛素的共组装体有望成为AD的一种可行治疗选择。

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