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解聚过程中生成的细胞毒性淀粉样寡聚物的结构。

Structure of cytotoxic amyloid oligomers generated during disaggregation.

机构信息

Department of Biotechnology and Life Science, Tokyo University of Agriculture and Technology, 2-24-16 Naka-cho, Koganei, Tokyo 184-8588, Japan.

出版信息

J Biochem. 2024 May 31;175(6):575-585. doi: 10.1093/jb/mvae023.

Abstract

Amyloidosis is characterized by the abnormal accumulation of amyloid proteins. The causative proteins aggregate from monomers to oligomers and fibrils, among which some intermediate oligomers are considered as major toxins. Cytotoxic oligomers are generated not only by aggregation but also via fibril disaggregation. However, little is known about the structural characteristics and generation conditions of cytotoxic oligomers produced during disaggregation. Herein, we summarized the structural commonalities of cytotoxic oligomers formed under various disaggregation conditions, including the addition of heat shock proteins or small compounds. In vitro experimental data demonstrated the presence of high-molecular-weight oligomers (protofibrils or protofilaments) that exhibited a fibrous morphology and β-sheet structure. Molecular dynamics simulations indicated that the distorted β-sheet structure contributed to their metastability. The tendency of these cytotoxic oligomers to appear under mild disaggregation conditions, implied formation during the early stages of disaggregation. This review will aid researchers in exploring the characteristics of highly cytotoxic oligomers and developing drugs that target amyloid aggregates.

摘要

淀粉样变性的特征是淀粉样蛋白的异常积聚。致病蛋白从单体聚集到低聚物和纤维,其中一些中间低聚物被认为是主要的毒素。细胞毒性低聚物不仅通过聚集产生,还通过纤维的解聚产生。然而,对于解聚过程中产生的细胞毒性低聚物的结构特征和产生条件知之甚少。本文总结了在各种解聚条件下形成的细胞毒性低聚物的结构共性,包括热休克蛋白或小分子化合物的添加。体外实验数据表明存在高分子量的寡聚物(原纤维或原丝),其具有纤维形态和β-折叠结构。分子动力学模拟表明,扭曲的β-折叠结构导致其亚稳性。这些细胞毒性低聚物在温和解聚条件下出现的趋势表明它们在解聚的早期阶段形成。这篇综述将有助于研究人员探索高细胞毒性低聚物的特性,并开发针对淀粉样蛋白聚集物的药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d77e/11155694/fcb7949b2329/mvae023ga.jpg

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