Decrease of prothrombin level during thrombolysis in acute myocardium infarction.

IF 1.4 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
Daria S Korolova, Alexander M Parkhomenko, Volodymyr Chernyshenko, Tamara M Chernyshenko, Nadiya M Druzhyna, Olha V Hornytska, Tetyana M Platonova
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引用次数: 0

Abstract

Previously, the direct interactions of Bβ26-42 fibrin residues with prothrombin were demonstrated. It was also shown that forming prothrombin complexes with E- or DDE-fragments causes non-enzymatic prothrombin activation. The direct measuring of the prothrombin level in the blood plasma of patients with acute myocardial infarction (AMI) allowed us to find a situation where such an activation can occur in vivo. Blood coagulation parameters in the blood plasma of patients with AMI were measured at 2 hours, three days, and seven days after the thrombolysis by streptokinase accompanied with intravenous administration of anticoagulants: unfractionated high molecular weight heparin (HMWH) and low-molecular-weight heparin (LMWH). The prothrombin level in the blood plasma of patients with AMI was normal before thrombolytic therapy and substantially decreased after streptokinase administration. This effect was prominent in the case of concomitant anticoagulant therapy with LMWH and was not observed when HMWH was applied. It can be explained by the fact that LMWH preferentially inhibits factor Xa, while the HMWH is an effective inhibitor of both factor Xa and thrombin. This observation suggested that the prothrombin level decrease was caused by the thrombin-like activity and possible autolysis of prothrombin by thrombin. Also, thrombolytic therapy with streptokinase caused the accumulation of fibrin degradation products (FDPs), some of which were able to bind prothrombin. The dramatic decrease of prothrombin level in the blood plasma of patients with AMI during thrombolysis allowed us to conclude the non-enzymatic prothrombin activation with the following autolysis of prothrombin that contributes to the pathology.

急性心肌梗死溶栓过程中凝血酶原水平的降低。
先前,已证实Bβ26-42纤维蛋白残基与凝血酶原的直接相互作用。研究还表明,与E-或dde片段形成凝血酶原复合物可引起非酶促凝血酶原活化。通过直接测量急性心肌梗死(AMI)患者血浆中的凝血酶原水平,我们发现了这种激活可以在体内发生的情况。AMI患者在链激酶溶栓后2小时、3天、7天分别测定血浆凝血参数,同时静脉给予抗凝剂:未分离的高分子量肝素(HMWH)和低分子量肝素(LMWH)。AMI患者溶栓前血浆凝血酶原水平正常,链激酶治疗后血浆凝血酶原水平明显下降。这种效果在与低分子肝素同时进行抗凝治疗的情况下表现突出,而在应用低分子肝素时未观察到。这可以解释为低分子肝素优先抑制Xa因子,而低分子肝素是Xa因子和凝血酶的有效抑制剂。这一观察结果表明,凝血酶原水平下降是由凝血酶样活性和凝血酶可能的自溶引起的。此外,用链激酶溶栓治疗引起纤维蛋白降解产物(fdp)的积累,其中一些能够结合凝血酶原。AMI患者在溶栓过程中血浆凝血酶原水平的急剧下降,使我们得出非酶促凝血酶原激活与随后的凝血酶原自溶是导致病理的原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Acta biochimica Polonica
Acta biochimica Polonica 生物-生化与分子生物学
CiteScore
2.40
自引率
0.00%
发文量
99
审稿时长
4-8 weeks
期刊介绍: Acta Biochimica Polonica is a journal covering enzymology and metabolism, membranes and bioenergetics, gene structure and expression, protein, nucleic acid and carbohydrate structure and metabolism.
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