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TrkB酪氨酸激酶中的顺式/反式顺序自磷酸化

Sequential cis/trans autophosphorylation in TrkB tyrosine kinase.

作者信息

Iwasaki Y, Nishiyama H, Suzuki K, Koizumi S

机构信息

Bio-Organic Research Department, Ciba-Geigy (Japan) Limited, Takarazuka.

出版信息

Biochemistry. 1997 Mar 4;36(9):2694-700. doi: 10.1021/bi962057x.

Abstract

TrkB, a member of the tyrosine kinase family of growth factor receptors, is activated by binding of brain-derived neurotrophic factor or neurotrophin 4/5. The intracellular kinase domain of TrkB (ICD-TrkB) was prepared by an insect cell expression system and characterized to identify the mechanism of autophosphorylation. The time course of autophosphorylation, which shows a biphasic progression with a slow nonlinear phase followed by a fast linear phase, indicates the existence of autophosphorylation-induced activation in ICD-TrkB. This is also supported by the finding that phosphorylated ICD-TrkB shows significantly higher activity than control naive ICD-TrkB. Interestingly, the autophosphorylation rate in the linear phase clearly depends on the ICD-TrkB concentration, whereas the rate of initial autophosphorylation is independent of the concentration of ICD-TrkB in the reaction mixture. This observation suggests a two-step autophosphorylation, first an intramolecular activating step and then an intermolecular step. This mechanism is confirmed by the result that only the later phase of autophos-phorylation is inhibited by addition of glycerol which interferes with intermolecular interactions. Therefore, we propose the mechanism of ICD-TrkB autophosphorylation as a sequential cis/trans phosphorylation.

摘要

TrkB是生长因子受体酪氨酸激酶家族的成员,通过与脑源性神经营养因子或神经营养蛋白4/5结合而被激活。TrkB的细胞内激酶结构域(ICD-TrkB)通过昆虫细胞表达系统制备,并对其进行表征以确定自磷酸化机制。自磷酸化的时间进程呈现双相进展,先是缓慢的非线性阶段,然后是快速的线性阶段,这表明ICD-TrkB中存在自磷酸化诱导的激活。磷酸化的ICD-TrkB比对照未处理的ICD-TrkB具有显著更高的活性这一发现也支持了这一点。有趣的是,线性阶段的自磷酸化速率明显取决于ICD-TrkB的浓度,而初始自磷酸化速率与反应混合物中ICD-TrkB的浓度无关。这一观察结果表明存在两步自磷酸化,首先是分子内激活步骤,然后是分子间步骤。通过添加甘油干扰分子间相互作用仅抑制自磷酸化后期这一结果证实了该机制。因此,我们提出ICD-TrkB自磷酸化机制为顺式/反式顺序磷酸化。

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