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酪氨酸74的硝化作用通过阻断半胱天冬酶-9的激活,阻止人细胞色素c在凋亡信号传导中发挥关键作用。

Nitration of tyrosine 74 prevents human cytochrome c to play a key role in apoptosis signaling by blocking caspase-9 activation.

作者信息

García-Heredia José M, Díaz-Moreno Irene, Nieto Pedro M, Orzáez Mar, Kocanis Stella, Teixeira Miguel, Pérez-Payá Enrique, Díaz-Quintana Antonio, De la Rosa Miguel A

机构信息

Instituto de Bioquímica Vegetal y Fotosíntesis, Universidad de Sevilla-CSIC, Avda. Americo Vespucio 49, Sevilla 41092, Spain.

出版信息

Biochim Biophys Acta. 2010 Jun-Jul;1797(6-7):981-93. doi: 10.1016/j.bbabio.2010.03.009. Epub 2010 Mar 20.

Abstract

Tyrosine nitration is one of the most common post-transcriptional modifications of proteins, so affecting their structure and function. Human cytochrome c, with five tyrosine residues, is an excellent case study as it is a well-known protein playing a double physiological role in different cell compartments. On one hand, it acts as electron carrier within the mitochondrial respiratory electron transport chain, and on the other hand, it serves as a cytoplasmic apoptosis-triggering agent. In a previous paper, we reported the effect of nitration on physicochemical and kinetic features of monotyrosine cytochrome c mutants. Here, we analyse the nitration-induced changes in secondary structure, thermal stability, haem environment, alkaline transition and molecular dynamics of three of such monotyrosine mutants--the so-called h-Y67, h-Y74 and h-Y97--which have four tyrosines replaced by phenylalanines and just keep the tyrosine residue giving its number to the mutant. The resulting data, along with the functional analyses of the three mutants, indicate that it is the specific nitration of solvent-exposed Tyr74 which enhances the peroxidase activity and blocks the ability of Cc to activate caspase-9, thereby preventing the apoptosis signaling pathway.

摘要

酪氨酸硝化是蛋白质最常见的转录后修饰之一,因此会影响其结构和功能。人细胞色素c有五个酪氨酸残基,是一个很好的研究案例,因为它是一种著名的蛋白质,在不同的细胞区室中发挥双重生理作用。一方面,它在线粒体呼吸电子传递链中作为电子载体,另一方面,它作为细胞质凋亡触发剂。在之前的一篇论文中,我们报道了硝化对单酪氨酸细胞色素c突变体的物理化学和动力学特征的影响。在这里,我们分析了三种单酪氨酸突变体(即所谓的h-Y67、h-Y74和h-Y97)在硝化诱导下二级结构、热稳定性、血红素环境、碱性转变和分子动力学的变化,这三种突变体中有四个酪氨酸被苯丙氨酸取代,只保留了赋予突变体编号的酪氨酸残基。所得数据以及这三种突变体的功能分析表明,溶剂暴露的Tyr74的特异性硝化增强了过氧化物酶活性,并阻断了细胞色素c激活caspase-9的能力,从而阻止了凋亡信号通路。

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