Unfractionated heparin inhibits thrombin-catalysed amplification reactions of coagulation more efficiently than those catalysed by factor Xa

C T Esmon; F A Ofosu; G J Modi; J Hirsh; J W Fenton; L M Smith; M A Blajchman; M R Buchanan; N Anvari

摘要

pWe have proposed previously that the steps in coagulation most sensitive to inhibition by heparin are the thrombin-dependent amplification reactions, and that prothrombinase is formed in heparinized plasma only after Factor Xa activates Factor VIII and Factor V. These propositions were based on the demonstration that both heparin and Phe-Pro-Arg-CH2Cl completely inhibited 125I-prothrombin activation for up to 60 s when contact-activated plasma (CAP) was replenished with Ca2+. Furthermore, the addition of thrombin to CAP before heparin or Phe-Pro-Arg-CH2Cl completely reversed their inhibitory effects. Additional support for the above hypotheses is provided in this study by demonstrating that, when the activity of thrombin is suppressed by heparin (indirectly) or by Phe-Pro-Arg-CH2Cl (directly), exogenous Factor Xa reverses the ability of these two agents to inhibit prothrombin activation. Prothrombin activation was initiated by adding Factor Xa (1 nM) or thrombin (1 or 10 nM) simultaneously with CaCl2 to CAP. In the absence of heparin or Phe-Pro-Arg-CH2Cl, prothrombin activation was seen 15 s later in either case. Heparin failed to delay, and Phe-Pro-Arg-CH2Cl delayed for 15 s, prothrombin activation in CAP supplemented with Factor Xa. In contrast, heparin and Phe-Pro-Arg-CH2Cl completely inhibited prothrombin activation for at least 45 s in CAP supplemented with 1 nM-thrombin. Heparin failed to delay prothrombin activation in CAP supplemented with 10 nM-thrombin, whereas Phe-Pro-Arg-CH2Cl completely inhibited prothrombin activation in this plasma for 45 s. These results suggest that in CAP: (1) Factor Xa can effectively activate Factor VIII and Factor V when the proteolytic activity of thrombin is suppressed; (2) heparin-antithrombin III is less able to inhibit Factor Xa than thrombin; (3) suppression of the thrombin-dependent amplification reactions is the primary anticoagulant effect of heparin./p

机译：>我们以前曾提出，对肝素抑制作用最敏感的凝血步骤是凝血酶依赖性扩增反应，凝血酶原酶只有在因子Xa激活因子VIII和因子V后才在肝素化血浆中形成。证明当补充接触激活的血浆（CAP）中的Ca2 +时，肝素和Phe-Pro-Arg-CH2Cl都能完全抑制125I-凝血酶原的激活长达60 s。此外，在肝素或Phe-Pro-Arg-CH2Cl之前在CAP中添加凝血酶可完全逆转其抑制作用。通过证明当肝素（间接）或Phe-Pro-Arg-CH2Cl（直接）抑制凝血酶的活性时，外源因子Xa逆转了这两种药物的能力，从而为上述假设提供了进一步的支持。抑制凝血酶原激活。凝血酶原激活可通过同时向CAP中添加因子Xa（1 nM）或凝血酶（1或10 nM）以及CaCl2来启动。在不存在肝素或Phe-Pro-Arg-CH2Cl的情况下，两种情况下均在15 s后发现凝血酶原活化。肝素未能延迟，Phe-Pro-Arg-CH2Cl延迟了15 s，凝血酶原在CAP中补充了Xa因子。相反，在补充了1 nM凝血酶的CAP中，肝素和Phe-Pro-Arg-CH2Cl完全抑制了凝血酶原激活至少45 s。肝素未能延迟补充有10 nM凝血酶的CAP中的凝血酶原激活，而Phe-Pro-Arg-CH2Cl在此血浆中完全抑制了凝血酶原激活45 s。这些结果表明在CAP中：（1）当凝血酶的蛋白水解活性受到抑制时，因子Xa可以有效地激活因子VIII和因子V; （2）肝素抗凝血酶III抑制凝血因子Xa的能力比凝血酶低。（3）抑制凝血酶依赖性扩增反应是肝素的主要抗凝作用。

Unfractionated heparin inhibits thrombin-catalysed amplification reactions of coagulation more efficiently than those catalysed by factor Xa

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