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谷氨酸纤溶酶原N端肽对谷氨酸纤溶酶原激活及其向赖氨酸纤溶酶原转化的影响。

Effects of N-terminal peptide of Glu-plasminogen on the activation of Glu-plasminogen and its conversion to Lys-plasminogen.

作者信息

Urano T, Takada Y, Takada A

机构信息

Department of Physiology, Hamamatsu University School of Medicine, Shizuoka-ken, Japan.

出版信息

Thromb Res. 1991 Feb 15;61(4):349-59. doi: 10.1016/0049-3848(91)90648-g.

Abstract

In order to analyze the mechanism of the intramolecular binding of the N-terminal peptide of Glu-plasminogen (Glu-plg) to its kringles, which results in its tight conformation, we synthesized peptides of the N-terminal portion of Glu-plg molecules and analyzed their effects on the activation of Glu-plg and its conversion to Lys-plasminogen (Lys-plg) by plasmin. Three peptides of Ala44-Lys50, Ala44-Glu51 and Ala44-Ser49 were synthesized in order to examine the effect of lysine residue in the peptide. Ala44-Lys50 and Ala44-Glu51 enhanced the activation of Glu-plg by urokinase, whereas the activation of Lys-plasminogen (Lys-plg) was slightly inhibited. The conversion of Glu-plg to Lys-plg by plasmin was also enhanced by these peptides. The results suggest that Ala44-Lys50 and Ala44-Glu51 worked on Glu-plg in a similar manner as lysine analogues by making its conformation looser. The third peptide Ala44-Ser49 did not have any effect on the activation of Glu-plg by urokinase or the conversion of Glu-plg to Lys-plg by plasmin. Ala44-Lys50 residue of Glu-plg is, therefore, strongly implicated as a candidate for the responsible site of the intramolecular binding in Glu-plg.

摘要

为了分析谷氨酸纤溶酶原(Glu-plg)的N端肽与其kringle结构域分子内结合的机制,该结合导致其紧密构象,我们合成了Glu-plg分子N端部分的肽,并分析了它们对Glu-plg激活以及纤溶酶将其转化为赖氨酸纤溶酶原(Lys-plg)的影响。合成了Ala44-Lys50、Ala44-Glu51和Ala44-Ser49三种肽,以研究肽中赖氨酸残基的作用。Ala44-Lys50和Ala44-Glu51增强了尿激酶对Glu-plg的激活作用,而对赖氨酸纤溶酶原(Lys-plg)的激活略有抑制。这些肽也增强了纤溶酶将Glu-plg转化为Lys-plg的过程。结果表明,Ala44-Lys50和Ala44-Glu51通过使Glu-plg的构象更松散,以与赖氨酸类似物相似的方式作用于Glu-plg。第三种肽Ala44-Ser49对尿激酶激活Glu-plg或纤溶酶将Glu-plg转化为Lys-plg没有任何影响。因此,Glu-plg的Ala44-Lys50残基被强烈认为是Glu-plg分子内结合的责任位点候选者。

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