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[特定配体诱导的肌肉糖原磷酸化酶b中迟缓的构象转变]

[Retarded conformational transitions in muscle glycogen phosphorylase b induced by specific ligands].

作者信息

Kurganov B I, Shchors E I, Livanova N B, Eronina T B, Chebotareva N A

出版信息

Biokhimiia. 1994 Apr;59(4):559-67.

PMID:8018778
Abstract

The effect of specific ligands on the initial rate of muscle glycogen phosphorylase b digestion by trypsin has been studied. The kinetics of tryptic proteolysis were followed by measuring the decrease in phosphorylase b fluorescence intensity at 335 nm (excitation at 290 nm). The kinetic curves were linear at least in the region 0-400 s (0.02 M HEPES, pH 6.8; 37 degrees C). An allosteric activator (AMP) and allosteric inhibitors (flavins) protected the enzyme from tryptic digestion when trypsin was added to the enzyme preincubated with the ligand. Differences were found between the kinetic curves of trypsinolysis initiated by addition of the trypsin-ligand mixture to phosphorylase b an by addition of trypsin to the enzyme preincubated with the ligand for 10 min. It is concluded that the specific ligands under study (AMP, flavins, and the substrate--glucose 1-phosphate) induce relatively slow conformational changes in the phosphorylase b molecule with the half-conversion time of several minutes.

摘要

研究了特定配体对胰蛋白酶消化肌肉糖原磷酸化酶b初始速率的影响。通过测量335nm处磷酸化酶b荧光强度的降低(激发波长为290nm)来跟踪胰蛋白酶解的动力学。动力学曲线至少在0-400s区域是线性的(0.02M HEPES,pH 6.8;37℃)。当将胰蛋白酶添加到与配体预孵育的酶中时,变构激活剂(AMP)和变构抑制剂(黄素)可保护该酶免受胰蛋白酶消化。在将胰蛋白酶-配体混合物添加到磷酸化酶b引发的胰蛋白酶解动力学曲线与将胰蛋白酶添加到与配体预孵育10分钟的酶引发的胰蛋白酶解动力学曲线之间发现了差异。得出的结论是,所研究的特定配体(AMP、黄素和底物——葡萄糖1-磷酸)在磷酸化酶b分子中诱导相对缓慢的构象变化,半转换时间为几分钟。

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