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组织型纤溶酶原激活剂可增加谷氨酸纤溶酶原与血栓的结合。

Tissue-type plasminogen activator increases the binding of glu-plasminogen to clots.

作者信息

Tran-Thang C, Kruithof E K, Bachmann F

出版信息

J Clin Invest. 1984 Dec;74(6):2009-16. doi: 10.1172/JCI111623.

Abstract

Porcine tissue-type plasminogen activator (t-PA) increases the binding of 125I-glu-plasminogen to clots made from human plasma or purified fibrinogen in a time and t-PA concentration dependent fashion. The accumulation of plasminogen was faster and greater on noncrosslinked plasma clots than on clots which had been crosslinked by Factor XIIIa. Furthermore, the uptake of plasminogen to crosslinked fibrin clots occurred at a slower rate in the presence of alpha 2-plasmin inhibitor (alpha 2 PI) than in its absence. The kinetics of the uptake of 125I-plasminogen were analyzed using SDS-polyacrylamide gel electrophoresis and radioautography of solubilized plasma clots formed in the presence of t-PA. During the initial phase there was a decrease of clot-bound glu-plasminogen; simultaneously, there was a slight increase in clot-bound glu-plasmin and in plasmin complexed to alpha 2 PI that was crosslinked to alpha-chain polymers of fibrin. This was followed by a marked increase in clot-bound plasminogen having glutamic acid as NH2-terminal (glu-plasminogen) and gluplasmin. t-PA-induced enhancement of glu-plasminogen uptake appears to be mediated by plasmin but does not require the conversion of glu-plasminogen to plasminogen having lysine or methionine as NH2-terminal. The described mechanism assures an adequate supply of clot-bound plasmin, which is the enzyme ultimately involved in the degradation of fibrin.

摘要

猪组织型纤溶酶原激活剂(t-PA)能以时间和t-PA浓度依赖性方式增加125I-谷氨酸纤溶酶原与人血浆或纯化纤维蛋白原制成的凝块的结合。纤溶酶原在非交联血浆凝块上的积累比经因子XIIIa交联的凝块更快且更多。此外,在存在α2-纤溶酶抑制剂(α2 PI)的情况下,纤溶酶原向交联纤维蛋白凝块的摄取速率比不存在时更慢。使用SDS-聚丙烯酰胺凝胶电泳和在t-PA存在下形成的溶解血浆凝块的放射自显影分析125I-纤溶酶原摄取的动力学。在初始阶段,凝块结合的谷氨酸纤溶酶原减少;同时,凝块结合的谷氨酸纤溶酶以及与交联到纤维蛋白α链聚合物的α2 PI复合的纤溶酶略有增加。随后,以谷氨酸为NH2末端的凝块结合纤溶酶原(谷氨酸纤溶酶原)和谷氨酸纤溶酶显著增加。t-PA诱导的谷氨酸纤溶酶原摄取增强似乎由纤溶酶介导,但不需要将谷氨酸纤溶酶原转化为以赖氨酸或蛋氨酸为NH2末端的纤溶酶原。所描述的机制确保了凝块结合纤溶酶的充足供应,而凝块结合纤溶酶是最终参与纤维蛋白降解的酶。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eda4/425389/39db82ca8e26/jcinvest00138-0131-a.jpg

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