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使用外位点抑制适体对蛋白酶激活蛋白C进行选择性调节。

Selective Modulation of the Protease Activated Protein C Using Exosite Inhibiting Aptamers.

作者信息

Hamedani Nasim Shahidi, Müller Jens, Tolle Fabian, Rühl Heiko, Pezeshkpoor Behnaz, Liphardt Kerstin, Oldenburg Johannes, Mayer Günter, Pötzsch Bernd

机构信息

Institute of Experimental Hematology and Transfusion Medicine, University of Bonn Medical Center, Bonn, Germany.

Life and Medical Sciences Institute, University of Bonn, Bonn, Germany.

出版信息

Nucleic Acid Ther. 2020 Oct;30(5):276-288. doi: 10.1089/nat.2020.0844. Epub 2020 Jun 2.

Abstract

Activated protein C (APC) is a serine protease with anticoagulant and cytoprotective activities. Nonanticoagulant APC mutants show beneficial effects as cytoprotective agents. To study, if such biased APC signaling can be achieved by APC-binding ligands, the aptamer technology has been used. A G-quadruplex-containing aptamer, G-NB3, has been selected that binds to the basic exosite of APC with a K of 0.2 nM and shows no binding to APC-related serine proteases or the zymogen protein C. G-NB3 inhibits the inactivation of activated cofactors V and VIII with IC values of 11.6 and 13.1 nM, respectively, without inhibiting the cytoprotective and anti-inflammatory functions of APC as tested using a staurosporine-induced apoptosis assay and a vascular barrier protection assay. In addition, G-NB3 prolongs the plasma half-life of APC through inhibition of APC-serine protease inhibitor complex formation. These physicochemical and functional characteristics qualify G-NB3 as a promising therapeutic agent usable to enhance the cytoprotective functions of APC without increasing the risk of APC-related hemorrhage.

摘要

活化蛋白C(APC)是一种具有抗凝和细胞保护活性的丝氨酸蛋白酶。非抗凝性APC突变体作为细胞保护剂显示出有益效果。为了研究是否可以通过APC结合配体实现这种偏向性APC信号传导,已使用适体技术。已筛选出一种含G-四链体的适体G-NB3,它以0.2 nM的解离常数(K)与APC的碱性外位点结合,且不与APC相关的丝氨酸蛋白酶或酶原蛋白C结合。G-NB3抑制活化辅因子V和VIII的失活,其半数抑制浓度(IC)分别为11.6和13.1 nM,在用星形孢菌素诱导的凋亡试验和血管屏障保护试验测试时,不抑制APC的细胞保护和抗炎功能。此外,G-NB3通过抑制APC-丝氨酸蛋白酶抑制剂复合物的形成来延长APC的血浆半衰期。这些物理化学和功能特性使G-NB3成为一种有前景的治疗剂,可用于增强APC的细胞保护功能而不增加与APC相关出血的风险。

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