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筛选针对淀粉样β肽的膜 RNA 适体:外泌体抗氧化策略的启示。

Selection of Membrane RNA Aptamers to Amyloid Beta Peptide: Implications for Exosome-Based Antioxidant Strategies.

机构信息

Institute of Biotechnology, University of Opole, Kominka 6, 45-032 Opole, Poland.

Department of MCD Biology, University of Colorado, Boulder, CO 80309, USA.

出版信息

Int J Mol Sci. 2019 Jan 13;20(2):299. doi: 10.3390/ijms20020299.

Abstract

The distribution of amyloid beta peptide 42 (Aβ42) between model exosomal membranes and a buffer solution was measured. The model membranes contained liquid-ordered regions or phosphatidylserine. Results demonstrated that up to ca. 20% of amyloid peptide, generated in the plasma (or intracellular) membrane as a result of proteolytic cleavage of amyloid precursor proteins by β- and γ-secretases, can stay within the membrane milieu. The selection of RNA aptamers that bind to Aβ42 incorporated into phosphatidylserine-containing liposomal membranes was performed using the selection-amplification (SELEX) method. After eight selection cycles, the pool of RNA aptamers was isolated and its binding to Aβ42-containing membranes was demonstrated using the gel filtration method. Since membranes can act as a catalytic surface for Aβ42 aggregation, these RNA aptamers may inhibit the formation of toxic amyloid aggregates that can permeabilize cellular membranes or disrupt membrane receptors. Strategies are proposed for using functional exosomes, loaded with RNA aptamers specific to membrane Aβ42, to reduce the oxidative stress in Alzheimer's disease and Down's syndrome.

摘要

测量了模型外体膜和缓冲溶液之间的淀粉样β肽 42(Aβ42)分布。该模型膜含有有序液体区域或磷脂酰丝氨酸。结果表明,多达约 20%的淀粉样肽可在血浆(或细胞内)膜中保留,这是由于β-和γ-分泌酶对淀粉样前体蛋白的蛋白水解切割而产生的。使用选择-扩增(SELEX)方法对与包含磷脂酰丝氨酸的脂质体膜结合的 Aβ42 进行 RNA 适体的选择。经过 8 个选择循环,分离 RNA 适体库,并使用凝胶过滤法证明其与 Aβ42 结合的膜结合。由于膜可以作为 Aβ42 聚集的催化表面,因此这些 RNA 适体可能会抑制形成有毒的淀粉样聚集物,从而破坏细胞膜或破坏膜受体。提出了使用载有针对膜 Aβ42 的 RNA 适体的功能性外体的策略,以减轻阿尔茨海默氏病和唐氏综合征中的氧化应激。

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