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具有两个抗凝血酶或血小板第4因子结合位点的肝素。

Heparin with two binding sites for antithrombin or platelet factor 4.

作者信息

Jordan R E, Favreau L V, Braswell E H, Rosenberg R D

出版信息

J Biol Chem. 1982 Jan 10;257(1):400-6.

PMID:7053378
Abstract

A new, highly discriminating affinity chromatographic technique has been developed which employs antithrombin and concanavalin A-Sepharose to fractionate heparin species of all molecular sizes. This methodology is able to subdivide the active mucopolysaccharide pools of molecular weight 6,000 to 8,000 (LMW) or 18,000 to 22,000 (HMW) into various species with descending affinities for antithrombin as well as decreasing anticoagulant potencies. The upper 10% of these two pools, either LMW or HMW highly active heparin, appears to be relatively homogeneous with respect to interactions with antithrombin and possessed anticoagulant potencies of 350 units/mg and 731 units/mg, respectively. The HMW highly active heparin has been examined by analytic ultracentrifugation. It exhibited a charge-connected weight-average molecular weight of 22,000 +/- 2,000 with minimal size heterogeneity. The stoichiometries of interaction of antithrombin and platelet factor 4 with HMW highly active heparin as determined by fluorescence spectroscopy indicated that 2 molecules of either protein are able to bind to 1 molecule of the mucopolysaccharide. These studies also reveal that the binding of antithrombin to HMW highly active heparin is characterized by KDISSHAT = 5.0 X 10(-8) M and KDISSHAT2 = 1.0 x 10(-7) M, respectively. The avidity of platelet factor 4 for HMW highly active heparin could not be quantitated but appears to be at least 10 to 100 times greater than that of antithrombin for mucopolysaccharide.

摘要

已开发出一种新型的、具有高度区分性的亲和色谱技术,该技术利用抗凝血酶和伴刀豆球蛋白A - 琼脂糖凝胶来分离所有分子大小的肝素种类。这种方法能够将分子量为6000至8000(低分子量)或18000至22000(高分子量)的活性黏多糖池细分为对抗凝血酶亲和力逐渐降低以及抗凝效力逐渐减弱的各种种类。这两个池的上部10%,即低分子量或高分子量高活性肝素,在与抗凝血酶的相互作用方面似乎相对均匀,抗凝效力分别为350单位/毫克和731单位/毫克。高分子量高活性肝素已通过分析超速离心法进行检测。它呈现出电荷连接的重均分子量为22000±2000,大小异质性最小。通过荧光光谱法测定,抗凝血酶和血小板因子4与高分子量高活性肝素相互作用的化学计量表明,这两种蛋白质的2个分子都能够与1个黏多糖分子结合。这些研究还表明,抗凝血酶与高分子量高活性肝素的结合分别以KDISSHAT = 5.0×10⁻⁸ M和KDISSHAT2 = 1.0×10⁻⁷ M为特征。无法对血小板因子4对高分子量高活性肝素的亲和力进行定量,但似乎比对黏多糖的抗凝血酶亲和力至少大10至100倍。

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