Ellis V, Scully M F, Kakkar V V
Biochem J. 1986 Jan 1;233(1):161-5. doi: 10.1042/bj2330161.
The influence of heparin on the inhibition of factor Xa has been studied under conditions where factor Xa is bound to collagen-thrombin-stimulated platelets to form the prothrombinase complex. Unfractionated heparin was found to cause a concentration-dependent acceleration of the inhibition of the platelet prothrombinase complex up to a maximum rate constant of 4.1 X 10(7) M-1 X min-1 at heparin concentrations of 0.2 microM and above. This is equivalent to a 4800-fold acceleration over the rate constant for the inhibition in the absence of heparin, and is 6.8-fold lower than the rate constant for the inhibition of uncomplexed factor Xa in the presence of saturating concentrations of heparin which was determined as 2.8 X 10(8) M-1 X min-1. The effects of three Mr fractions of heparin were also studied. These were a gel-filtered heparin of Mr 15000, a gel-filtered heparin of Mr 6000 and a heparin oligosaccharide (primarily 8-10 monosaccharide units) prepared by nitrous acid depolymerization, each with high affinity for antithrombin III. These fractions all accelerated the rate of the antithrombin III inhibition of the platelet prothrombinase complex, with maximum rate constants of 6.8 X 10(7), 1.4 X 10(7) and 9.8 X 10(6) M-1 X min-1, respectively. On comparison with the effect of these heparin fractions on the rate of inhibition of uncomplexed factor Xa a progressively increasing disparity between the rate of inhibition of uncomplexed and complexed factor Xa was observed, rising from 1.7-fold with the oligosaccharide to 6.8-fold with the unfractionated heparin. A possible mechanism for this differential activity between uncomplexed and complexed factor Xa with the various heparin fractions is discussed in terms of an involvement of heparin binding to factor Xa.
在因子Xa与胶原-凝血酶刺激的血小板结合形成凝血酶原酶复合物的条件下,研究了肝素对因子Xa抑制作用的影响。发现未分级肝素会导致血小板凝血酶原酶复合物抑制作用呈浓度依赖性加速,在肝素浓度为0.2微摩尔及以上时,最大速率常数为4.1×10⁷ M⁻¹×分钟⁻¹。这相当于在无肝素情况下抑制速率常数的4800倍加速,且比在肝素饱和浓度下抑制未复合因子Xa的速率常数低6.8倍,后者测定为2.8×10⁸ M⁻¹×分钟⁻¹。还研究了肝素的三个分子量级分的作用。它们分别是分子量为15000的凝胶过滤肝素、分子量为6000的凝胶过滤肝素以及通过亚硝酸解聚制备的肝素寡糖(主要为8 - 10个单糖单元),每种对抗凝血酶III都有高亲和力。这些级分均加速了抗凝血酶III对血小板凝血酶原酶复合物的抑制速率,最大速率常数分别为6.8×10⁷、1.4×10⁷和9.8×10⁶ M⁻¹×分钟⁻¹。与这些肝素级分对未复合因子Xa抑制速率的作用相比,观察到未复合和复合因子Xa抑制速率之间的差异逐渐增大,从寡糖的1.7倍增加到未分级肝素的6.8倍。根据肝素与因子Xa结合的参与情况,讨论了未复合和复合因子Xa与各种肝素级分之间这种差异活性的可能机制。