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三种不同的三硫键连接的 tridegin 异构体可差异抑制凝血因子 XIIIa:结构稳定性对生物活性的影响。

Distinct 3-disulfide-bonded isomers of tridegin differentially inhibit coagulation factor XIIIa: The influence of structural stability on bioactivity.

机构信息

Pharmaceutical Biochemistry and Bioanalytics, Pharmaceutical Institute, University of Bonn, An der Immenburg 4, D-53121, Bonn, Germany.

Institute II of Pharmacology, Center of Pharmacology, Medical Faculty, University of Cologne, Gleueler Str. 24, D-50931, Cologne, Germany.

出版信息

Eur J Med Chem. 2020 Sep 1;201:112474. doi: 10.1016/j.ejmech.2020.112474. Epub 2020 May 23.

Abstract

Tridegin is a 66mer cysteine-rich coagulation factor XIIIa (FXI-IIa) inhibitor from the giant amazon leech Haementeria ghilianii of yet unknown disulfide connectivity. This study covers the structural and functional characterization of five different 3-disulfide-bonded tridegin isomers. In addition to three previously identified isomers, one isomer containing the inhibitory cystine knot (ICK, knottin) motif, and one isomer with the leech antihemostatic protein (LAP) motif were synthesized in a regioselective manner. A fluorogenic enzyme activity assay revealed a positive correlation between the constriction of conformational flexibility in the N-terminal part of the peptide and the inhibitory potential towards FXI-IIa with clear differences between the isomers. This observation was supported by molecular dynamics (MD) simulations and subsequent molecular docking studies. The presented results provide detailed structure-activity relationship studies of different tridegin disulfide isomers towards FXI-IIa and reveal insights into the possibly existing native linkage compared to non-native disulfide tridegin species.

摘要

Tridegin 是一种富含半胱氨酸的凝血因子 XIIIa (FXI-IIa) 抑制剂,来自巨型亚马逊水蛭 Haementeria ghilianii,其二硫键连接方式尚不清楚。本研究涵盖了五种不同的三硫键结合 tridegin 异构体的结构和功能表征。除了之前鉴定的三种异构体外,还以区域选择性的方式合成了一种含有抑制性半胱氨酸结(ICK,knottin)基序的异构体和一种具有水蛭抗止血蛋白(LAP)基序的异构体。荧光酶活性测定表明,肽的 N 端部分构象灵活性的收缩与对 FXI-IIa 的抑制潜力呈正相关,不同异构体之间存在明显差异。这一观察结果得到了分子动力学 (MD) 模拟和随后的分子对接研究的支持。所呈现的结果提供了针对 FXI-IIa 的不同 tridegin 二硫键异构体的详细结构-活性关系研究,并揭示了与非天然二硫键 tridegin 物种相比,天然存在的连接的可能性。

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