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防御素可调节组织型纤溶酶原激活物及纤溶酶原与纤维蛋白和内皮细胞的结合。

Defensin modulates tissue-type plasminogen activator and plasminogen binding to fibrin and endothelial cells.

作者信息

Higazi A A, Ganz T, Kariko K, Cines D B

机构信息

Department of Pathology, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Biol Chem. 1996 Jul 26;271(30):17650-5. doi: 10.1074/jbc.271.30.17650.

DOI:10.1074/jbc.271.30.17650
PMID:8663495
Abstract

Defensins are naturally occurring antimicrobial peptides that may participate in host defense against microorganisms. We previously reported that the amino acid sequence of leukocyte defensins resembles the lysine-binding site in the kringles of plasminogen and that defensin inhibits fibrinolysis mediated by tissue-type plasminogen activator (tPA) and plasminogen. In the present paper we analyze the mechanisms of this inhibition. Defensin binds specifically to cultured human umbilical vein endothelial cells (HUVEC) (half-maximal binding = 3 microM) as well as to fibrin. At saturating concentrations (5-10 microM), defensin stimulates the maximum binding of plasminogen to HUVEC and to fibrin approximately 10-fold. However, defensin inhibits plasminogen binding to both surfaces at concentrations >10 microM. Defensin also inhibits tPA and plasminogen-mediated fibrinolysis in a dose-dependent manner at all concentrations tested. Fibrinolysis is almost totally inhibited by 6 microM defensin, a concentration that stimulates the binding of plasminogen to fibrin. Discordance between the enhancement of plasminogen binding and its activation cannot be explained by an inhibitory effect of defensin on tPA binding nor by inhibition of plasmin activity, each of which occur only at higher concentrations. Rather, these results suggest that plasminogen bound to fibrin in the presence of defensin is less susceptible to activation by tPA.

摘要

防御素是天然存在的抗菌肽,可能参与宿主对微生物的防御。我们之前报道过,白细胞防御素的氨基酸序列类似于纤溶酶原kringle结构域中的赖氨酸结合位点,并且防御素可抑制组织型纤溶酶原激活物(tPA)和纤溶酶原介导的纤维蛋白溶解。在本文中,我们分析了这种抑制作用的机制。防御素可特异性结合培养的人脐静脉内皮细胞(HUVEC)(半数最大结合浓度 = 3 microM)以及纤维蛋白。在饱和浓度(5 - 10 microM)下,防御素可使纤溶酶原与HUVEC和纤维蛋白的最大结合增加约10倍。然而,当浓度>10 microM时,防御素会抑制纤溶酶原与这两种表面的结合。在所有测试浓度下,防御素还以剂量依赖的方式抑制tPA和纤溶酶原介导的纤维蛋白溶解。6 microM的防御素几乎完全抑制了纤维蛋白溶解,而该浓度可刺激纤溶酶原与纤维蛋白的结合。纤溶酶原结合增强与其激活之间的不一致,既不能用防御素对tPA结合的抑制作用来解释,也不能用对纤溶酶活性的抑制来解释,因为这两种情况都仅在较高浓度时才会发生。相反,这些结果表明,在防御素存在的情况下,与纤维蛋白结合的纤溶酶原对tPA激活的敏感性较低。

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