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纤维蛋白原片段D对纤维蛋白组装抑制作用的表征

Characterization of the inhibition of fibrin assembly by fibrinogen fragment D.

作者信息

Williams J E, Hantgan R R, Hermans J, McDonagh J

出版信息

Biochem J. 1981 Sep 1;197(3):661-8. doi: 10.1042/bj1970661.

Abstract

Fragment D (Mr 100 000) prepared from a terminal plasmin digest of fibrinogen was isolated and used to study its effect on fibrin formation. Increasing amounts of fragment D added to a solution of fibrinogen and thrombin decrease the rigidity of the resultant gel (10% of control at 2 mol of fragment D/mol of fibrinogen). Half-maximal inhibition is achieved at 1 mol of fragment D/mol of fibrinogen for non-cross-linked clots and at 1/2 mol of fragment D/mol of fibrinogen for cross-linked clots. "Clottability' decreases concomitantly with the rigidity. Only small amounts of fragment D (less than 10% for non-cross-linked gels) are incorporated into the gel. Light-scattering shows an increase in the final fibre thickness at fragment D concentrations up to 2 mol of fragment D/mol of fibrinogen, from 60 molecules/cross-section for the control to 120 molecules/cross-section. Higher fragment D concentrations lead to a decrease in the final fibre thickness. The limit fibre thickness is 8 nm, with a length of 80 nm, which is equivalent to a fibrin trimer. On the basis of results of synthetic-substrate and fibrinopeptide-release assays, it is clear that thrombin inactivation is not responsible for this effect. These data suggest that fragment D may inhibit fibrin formation by blocking the bimolecular polymerization of activated fibrin monomer molecules to form protofibrils, although additional effects on subsequent assembly steps may also be involved.

摘要

从纤维蛋白原的终末纤溶酶消化产物中制备出片段D(分子量100 000),将其分离出来并用于研究其对纤维蛋白形成的影响。向纤维蛋白原和凝血酶溶液中添加越来越多的片段D会降低所得凝胶的硬度(在片段D与纤维蛋白原的摩尔比为2时,硬度为对照的10%)。对于非交联凝块,在片段D与纤维蛋白原的摩尔比为1时达到半数最大抑制,对于交联凝块,在片段D与纤维蛋白原的摩尔比为1/2时达到半数最大抑制。“凝块形成能力”随硬度的降低而相应下降。只有少量的片段D(对于非交联凝胶,小于10%)掺入凝胶中。光散射显示,在片段D浓度高达片段D与纤维蛋白原的摩尔比为2时,最终纤维厚度增加,从对照的每横截面60个分子增加到每横截面120个分子。更高的片段D浓度会导致最终纤维厚度减小。极限纤维厚度为8纳米,长度为80纳米,相当于一个纤维蛋白三聚体。根据合成底物和纤维蛋白肽释放试验的结果,很明显这种作用不是由凝血酶失活引起的。这些数据表明,片段D可能通过阻断活化的纤维蛋白单体分子的双分子聚合以形成原纤维来抑制纤维蛋白形成,尽管可能也涉及对后续组装步骤的其他影响。

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本文引用的文献

1
The Mechanism of Polymerization of Fibrinogen.纤维蛋白原的聚合机制
Proc Natl Acad Sci U S A. 1952 Jul;38(7):566-9. doi: 10.1073/pnas.38.7.566.

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