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利用计算机设计的适体探测 TDP-43 凝聚

Probing TDP-43 condensation using an in silico designed aptamer.

机构信息

Centre for Human Technologies (CHT), Istituto Italiano di Tecnologia (IIT), Via Enrico Melen, 83, 16152, Genova, Italy.

EaStCHEM School of Chemistry, University of Edinburgh, Edinburgh, EH9 3FJ, UK.

出版信息

Nat Commun. 2022 Jun 23;13(1):3306. doi: 10.1038/s41467-022-30944-x.

Abstract

Aptamers are artificial oligonucleotides binding to specific molecular targets. They have a promising role in therapeutics and diagnostics but are often difficult to design. Here, we exploited the catRAPID algorithm to generate aptamers targeting TAR DNA-binding protein 43 (TDP-43), whose aggregation is associated with Amyotrophic Lateral Sclerosis. On the pathway to forming insoluble inclusions, TDP-43 adopts a heterogeneous population of assemblies, many smaller than the diffraction-limit of light. We demonstrated that our aptamers bind TDP-43 and used the tightest interactor, Apt-1, as a probe to visualize TDP-43 condensates with super-resolution microscopy. At a resolution of 10 nanometers, we tracked TDP-43 oligomers undetectable by standard approaches. In cells, Apt-1 interacts with both diffuse and condensed forms of TDP-43, indicating that Apt-1 can be exploited to follow TDP-43 phase transition. The de novo generation of aptamers and their use for microscopy opens a new page to study protein condensation.

摘要

适体是与特定分子靶标结合的人工寡核苷酸。它们在治疗学和诊断学中有很好的应用前景,但设计起来通常很困难。在这里,我们利用 catRAPID 算法来生成针对 TAR DNA 结合蛋白 43(TDP-43)的适体,TDP-43 的聚集与肌萎缩侧索硬化症有关。在形成不溶性包涵体的过程中,TDP-43 采用了多种组装体,其中许多比光的衍射极限小。我们证明了我们的适体可以与 TDP-43 结合,并使用最紧密的相互作用体 Apt-1 作为探针,用超分辨率显微镜可视化 TDP-43 凝聚物。在 10 纳米的分辨率下,我们跟踪了标准方法无法检测到的 TDP-43 低聚物。在细胞中,Apt-1 与 TDP-43 的弥散和凝聚形式相互作用,表明 Apt-1 可用于跟踪 TDP-43 相变。适体的从头生成及其在显微镜中的应用为研究蛋白质凝聚开辟了新的一页。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/494c/9226187/b0f2b8b91802/41467_2022_30944_Fig1_HTML.jpg

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