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蜱源库尼茨型抑制剂作为抗止血因子。

Tick-derived Kunitz-type inhibitors as antihemostatic factors.

作者信息

Corral-Rodríguez María Angeles, Macedo-Ribeiro Sandra, Barbosa Pereira Pedro José, Fuentes-Prior Pablo

机构信息

Institut de Recerca, Hospital de la Santa Creu i Sant Pau, Sant Antoni Maria Claret 167, 08025 Barcelona, Spain.

出版信息

Insect Biochem Mol Biol. 2009 Sep;39(9):579-95. doi: 10.1016/j.ibmb.2009.07.003. Epub 2009 Jul 24.

DOI:10.1016/j.ibmb.2009.07.003
PMID:19631744
Abstract

Endogenous Kunitz-type inhibitors target a large number of serine proteinases, including coagulation factors VIIa and Xa, but not thrombin. By contrast, several two-domain Kunitz inhibitors of this major procoagulant proteinase have been isolated from both soft ticks (e.g., ornithodorin from Ornithodoros moubata) and hard ticks (e.g., boophilin from Rhipicephalus (Boophilus) microplus). Surprisingly, these anticoagulants do not follow the canonical mechanism of proteinase inhibition. Instead, their N-terminal residues bind across the thrombin active-site cleft, while C-terminal modules interact with the basic exosite I. The reactive-site loop of boophilin remains fully accessible in its complex with thrombin, and might interact with FXa according to the standard mechanism. A conceptually similar inhibition mechanism is employed by a related inhibitor of the TF-FVIIa complex isolated from Ixodes scapularis, ixolaris. Significant variations to the Kunitz fold are encountered in several of these factors, and are particularly evident in the single-domain FXa inhibitor, O. moubata TAP, and in soft tick-derived platelet antiaggregants (e.g., O. moubata disagregin). Altogether, these antihemostatic factors illustrate the divergence between hard and soft ticks. The unsurpassed versatility of tick-derived Kunitz inhibitors establishes them as valuable tools for biochemical investigations, but also as lead compounds for the development of novel antithrombotics.

摘要

内源性库尼茨型抑制剂作用于大量丝氨酸蛋白酶,包括凝血因子VIIa和Xa,但不作用于凝血酶。相比之下,已从软蜱(如来自莫氏钝缘蜱的钝缘蜱素)和硬蜱(如来自微小牛蜱的牛蜱抗凝蛋白)中分离出几种作用于这种主要促凝蛋白酶的双结构域库尼茨抑制剂。令人惊讶的是,这些抗凝剂并不遵循蛋白酶抑制的经典机制。相反,它们的N端残基横跨凝血酶活性位点裂隙结合,而C端模块与碱性外位点I相互作用。牛蜱抗凝蛋白的反应位点环在其与凝血酶的复合物中仍完全可及,并可能根据标准机制与因子Xa相互作用。从肩突硬蜱分离出的组织因子 - VIIa复合物的相关抑制剂艾索拉利,采用了概念上类似的抑制机制。在这些因子中的几种中,库尼茨折叠存在显著变异,在单结构域因子Xa抑制剂莫氏钝缘蜱TAP和软蜱来源的血小板抗聚集剂(如莫氏钝缘蜱解聚素)中尤为明显。总之,这些抗止血因子说明了硬蜱和软蜱之间的差异。蜱源库尼茨抑制剂无与伦比的多功能性使其成为生化研究的宝贵工具,也是开发新型抗血栓药物的先导化合物。

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