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肝素辅因子II与凝血酶相互作用及抗凝血酶III与凝血酶相互作用中肝素刺激的分子量依赖性比较。

Comparison of the molecular mass dependency of heparin stimulation of heparin cofactor II:thrombin interaction to antithrombin III:thrombin interaction.

作者信息

Scully M F, Ellis V, Kakkar V V

出版信息

Thromb Res. 1987 May 1;46(3):491-502. doi: 10.1016/0049-3848(87)90136-8.

Abstract

The influence of increasing concentrations of heparin of different molecular mass (Mr) has been compared in potentiation of the rate of heparin cofactor II:thrombin interaction and of antithrombin III:thrombin interaction. Unfractionated and fractionated heparin showed a concentration dependent ascending and descending limb of stimulation of the rate for both inhibitors. Unfractionated heparin and fractions of 16.5 KDa or less showed a peak acceleration of the rate of interaction of thrombin with both inhibitors at 0.3 X 10(-6) M heparin although the observed maximum rate at this peak decreased with fall in Mr. For both inhibitors two high Mr fractions showed peak stimulation at a lower heparin concentration (0.3 X 10(-7) M) and approximately two-fold greater increase in rate than that observed with unfractionated heparin. Potentiation of heparin cofactor II inhibitory activity differed from that of antithrombin III in that it was reversed by lower ionic strength and was not reversed by a heparin pentasaccharide with high affinity for antithrombin III. It is proposed that differences in the profiles of stimulation by high Mr fractions to those of lower Mr are related to higher binding affinities for the inhibitor permitting maximal binding of heparin before the descending part of the slope due to saturation of thrombin (according to the template hypothesis).

摘要

已比较了不同分子量(Mr)的肝素浓度增加对增强肝素辅因子II与凝血酶相互作用速率以及抗凝血酶III与凝血酶相互作用速率的影响。未分级肝素和分级肝素对两种抑制剂的刺激速率均呈现浓度依赖性的上升和下降阶段。未分级肝素以及16.5 kDa及以下的分级肝素在0.3×10⁻⁶ M肝素时,凝血酶与两种抑制剂相互作用的速率出现峰值加速,尽管在此峰值处观察到的最大速率随分子量降低而下降。对于两种抑制剂,两个高分子量分级肝素在较低的肝素浓度(0.3×10⁻⁷ M)时显示出峰值刺激,且速率增加约为未分级肝素的两倍。肝素辅因子II抑制活性的增强与抗凝血酶III不同,因为它在较低离子强度下会逆转,且不会被对抗凝血酶III具有高亲和力的肝素五糖逆转。据推测,高分子量分级肝素与低分子量分级肝素刺激曲线的差异与对抑制剂的更高结合亲和力有关,这使得在由于凝血酶饱和导致斜率下降部分之前,肝素能够实现最大结合(根据模板假说)。

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