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使用混合L-RNA/L-DNA适体靶向补体过敏毒素C5a的结构基础。

Structural basis for the targeting of complement anaphylatoxin C5a using a mixed L-RNA/L-DNA aptamer.

作者信息

Yatime Laure, Maasch Christian, Hoehlig Kai, Klussmann Sven, Andersen Gregers R, Vater Axel

机构信息

Department of Molecular Biology and Genetics, Aarhus University, Gustav Wieds Vej 10C, DK-8000 Aarhus, Denmark.

NOXXON Pharma AG, Max-Dohrn-Strasse 8-10, 10589 Berlin, Germany.

出版信息

Nat Commun. 2015 Apr 22;6:6481. doi: 10.1038/ncomms7481.

Abstract

L-Oligonucleotide aptamers (Spiegelmers) consist of non-natural L-configured nucleotides and are of particular therapeutic interest due to their high resistance to plasma nucleases. The anaphylatoxin C5a, a potent inflammatory mediator generated during complement activation that has been implicated with organ damage, can be efficiently targeted by Spiegelmers. Here, we present the first crystallographic structures of an active Spiegelmer, NOX-D20, bound to its physiological targets, mouse C5a and C5a-desArg. The structures reveal a complex 3D architecture for the L-aptamer that wraps around C5a, including an intramolecular G-quadruplex stabilized by a central Ca(2+) ion. Functional validation of the observed L-aptamer:C5a binding mode through mutational studies also rationalizes the specificity of NOX-D20 for mouse and human C5a against macaque and rat C5a. Finally, our structural model provides the molecular basis for the Spiegelmer affinity improvement through positional L-ribonucleotide to L-deoxyribonucleotide exchanges and for its inhibition of the C5a:C5aR interaction.

摘要

L-寡核苷酸适配体(镜像寡核苷酸)由非天然的L构型核苷酸组成,由于其对血浆核酸酶具有高度抗性,因此具有特殊的治疗意义。过敏毒素C5a是补体激活过程中产生的一种强效炎症介质,与器官损伤有关,可被镜像寡核苷酸有效靶向。在此,我们展示了活性镜像寡核苷酸NOX-D20与其生理靶点小鼠C5a和C5a-去精氨酸结合的首个晶体结构。这些结构揭示了L-适配体围绕C5a的复杂三维结构,包括由中心Ca(2+)离子稳定的分子内G-四链体。通过突变研究对观察到的L-适配体:C5a结合模式进行功能验证,也解释了NOX-D20对小鼠和人C5a相对于猕猴和大鼠C5a的特异性。最后,我们的结构模型为通过L-核糖核苷酸到L-脱氧核糖核苷酸的位置交换提高镜像寡核苷酸亲和力及其对C5a:C5aR相互作用的抑制提供了分子基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aa51/4423239/468bf5d02646/ncomms7481-f1.jpg

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