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基于纳米伴侣的策略控制与构象疾病相关的蛋白质聚集。

Nanochaperone-Based Strategies to Control Protein Aggregation Linked to Conformational Diseases.

机构信息

nanoBIC, Departament de Química Inorgànica i Orgànica, Universitat de Barcelona, Martí i Franquès, 1-11, 08028, Barcelona, Spain.

Institute of Nanoscience and Nanotechnology (IN2UB), Universitat de Barcelona, 08028, Barcelona, Spain.

出版信息

Angew Chem Int Ed Engl. 2021 Jan 4;60(1):41-52. doi: 10.1002/anie.202007924. Epub 2020 Aug 20.

Abstract

The generation of highly organized amyloid fibrils is associated with a wide range of conformational pathologies, including primarily neurodegenerative diseases. Such disorders are characterized by misfolded proteins that lose their normal physiological roles and acquire toxicity. Recent findings suggest that proteostasis network impairment may be one of the causes leading to the accumulation and spread of amyloids. These observations are certainly contributing to a new focus in anti-amyloid drug design, whose efforts are so far being centered on single-target approaches aimed at inhibiting amyloid aggregation. Chaperones, known to maintain proteostasis, hence represent interesting targets for the development of novel therapeutics owing to their potential protective role against protein misfolding diseases. In this minireview, research on nanoparticles that can either emulate or help molecular chaperones in recognizing and/or correcting protein misfolding is discussed. The nascent concept of "nanochaperone" may indeed set future directions towards the development of cost-effective, disease-modifying drugs to treat several currently fatal disorders.

摘要

高度组织的淀粉样纤维的产生与广泛的构象病理学有关,包括主要的神经退行性疾病。这些疾病的特征是蛋白质错误折叠,失去正常的生理功能,并获得毒性。最近的发现表明,蛋白质稳态网络的损伤可能是导致淀粉样蛋白积累和扩散的原因之一。这些观察结果无疑为抗淀粉样蛋白药物设计提供了一个新的重点,迄今为止,这些努力主要集中在旨在抑制淀粉样蛋白聚集的单一靶点方法上。伴侣蛋白,已知能维持蛋白质稳态,因此由于其对蛋白质错误折叠疾病的潜在保护作用,代表了开发新型治疗药物的有趣靶点。在这篇简评中,讨论了可以模拟或帮助分子伴侣识别和/或纠正蛋白质错误折叠的纳米颗粒的研究。“纳米伴侣”这一新兴概念确实为开发具有成本效益的、可改变疾病的药物以治疗目前几种致命疾病指明了未来的方向。

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