Dynamics in Redox-Active Molecules Following Ischemic Preconditioning in the Brain

IF 3.2 Q2 CLINICAL NEUROLOGY Neurology International Pub Date : 2024-05-09 DOI:10.3390/neurolint16030040
T. Lysikova, A. Tomašcová, M. Kovalska, J. Lehotský, Katarina Leskova Majdova, Peter Kaplán, Z. Tatarkova
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Abstract

It is well known that the brain is quite vulnerable to oxidative stress, initiating neuronal loss after ischemia-reperfusion (IR) injury. A potent protective mechanism is ischemic preconditioning (IPC), where proteins are among the primary targets. This study explores redox-active proteins’ role in preserving energy supply. Adult rats were divided into the control, IR, and IPC groups. Protein profiling was conducted to identify modified proteins and then verified through activity assays, immunoblot, and immunohistochemical analyses. IPC protected cortex mitochondria, as evidenced by a 2.26-fold increase in superoxide dismutase (SOD) activity. Additionally, stable core subunits of respiratory chain complexes ensured sufficient energy production, supported by a 16.6% increase in ATP synthase activity. In hippocampal cells, IPC led to the downregulation of energy-related dehydrogenases, while a significantly higher level of peroxiredoxin 6 (PRX6) was observed. Notably, IPC significantly enhanced glutathione reductase activity to provide sufficient glutathione to maintain PRX6 function. Astrocytes may mobilize PRX6 to protect neurons during initial ischemic events, by decreased PRX6 positivity in astrocytes, accompanied by an increase in neurons following both IR injury and IPC. Maintained redox signaling via astrocyte-neuron communication triggers IPC’s protective state. The partnership among PRX6, SOD, and glutathione reductase appears essential in safeguarding and stabilizing the hippocampus.
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脑缺血预处理后氧化还原活性分子的动态变化
众所周知,大脑很容易受到氧化应激的影响,缺血再灌注(IR)损伤后会导致神经元丧失。一种有效的保护机制是缺血预处理(IPC),其中蛋白质是主要靶点之一。本研究探讨了氧化还原活性蛋白质在保护能量供应方面的作用。成年大鼠被分为对照组、IR 组和 IPC 组。研究人员对蛋白质进行了分析,以确定被修饰的蛋白质,然后通过活性测定、免疫印迹和免疫组化分析进行验证。超氧化物歧化酶 (SOD) 活性增加了 2.26 倍,证明 IPC 保护了大脑皮层线粒体。此外,稳定的呼吸链复合物核心亚基确保了足够的能量产生,ATP 合酶活性增加了 16.6%。在海马细胞中,IPC 导致与能量相关的脱氢酶下调,同时观察到过氧化物歧化酶 6 (PRX6) 的水平显著提高。值得注意的是,IPC 能显著提高谷胱甘肽还原酶的活性,从而提供足够的谷胱甘肽来维持 PRX6 的功能。在最初的缺血事件中,星形胶质细胞可能会动员 PRX6 来保护神经元,因为在红外损伤和 IPC 之后,星形胶质细胞中 PRX6 阳性降低,而神经元中 PRX6 阳性升高。通过星形胶质细胞-神经元通信维持氧化还原信号触发了 IPC 的保护状态。PRX6、SOD和谷胱甘肽还原酶之间的伙伴关系似乎对保护和稳定海马至关重要。
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来源期刊
Neurology International
Neurology International CLINICAL NEUROLOGY-
CiteScore
3.70
自引率
3.30%
发文量
69
审稿时长
11 weeks
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