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通过对纤维蛋白肽释放动力学的研究比较各种人纤维蛋白原及其衍生物的结构。

Comparison of structures of various human fibrinogens and a derivative thereof by a study of the kinetics of release of fibrinopeptides.

作者信息

Hanna L S, Scheraga H A, Francis C W, Marder V J

出版信息

Biochemistry. 1984 Sep 25;23(20):4681-7. doi: 10.1021/bi00315a025.

Abstract

The kinetics of the thrombin-induced release of fibrinopeptides from several variants of human fibrinogen, and from the plasmin digestion fragment E thereof, have been studied by using an HPLC technique to separate the reaction products. The data were analyzed in terms of a Michaelis-Menten mechanism in which the A alpha and B beta chains compete for thrombin. Phosphorylation of Ser-3 of the A alpha chain appears to increase the rate of release of the corresponding phosphorylated peptide A from fibrinogen, due to enhanced binding of thrombin (lower value of the Michaelis-Menten constant KM). However, phosphorylation does not affect the rate of release of the unphosphorylated A or B peptides. Increase in the length of the gamma chain (at the C-terminus) does not affect the rate of release of any of the fibrinopeptides. The rate of release of the A peptide from fragment E (which is devoid of the B peptide) is similar to that for the complete fibrinogen molecule. These results are in agreement with an earlier conclusion [Martinelli, R. A., & Scheraga, H. A. (1980) Biochemistry 19, 2343] that the A alpha and B beta chains behave independently in their competition for thrombin; i.e., the hydrolyzable Arg-Gly bonds of the A alpha and B beta chains are both accessible to thrombin.

摘要

利用高效液相色谱(HPLC)技术分离反应产物,研究了凝血酶诱导几种人纤维蛋白原变体及其纤溶酶消化片段E释放纤维蛋白肽的动力学。根据米氏(Michaelis-Menten)机制对数据进行分析,其中Aα链和Bβ链竞争凝血酶。Aα链的Ser-3磷酸化似乎会增加纤维蛋白原中相应磷酸化肽A的释放速率,这是由于凝血酶结合增强(米氏常数KM值降低)。然而,磷酸化并不影响未磷酸化的A肽或B肽的释放速率。γ链(在C末端)长度的增加不影响任何纤维蛋白肽的释放速率。片段E(不含B肽)中A肽的释放速率与完整纤维蛋白原分子的相似。这些结果与早期的结论[Martinelli, R. A., & Scheraga, H. A. (1980) Biochemistry 19, 2343]一致,即Aα链和Bβ链在竞争凝血酶时表现独立;也就是说,Aα链和Bβ链的可水解Arg-Gly键对凝血酶都是可及的。

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