Sirtuins modulators mitigate hypoxia-induced cell death due to changes in histone 3 acetylation, and mitochondrial function, dynamics, and content

IF 4.6 2区医学 Q1 NEUROSCIENCES

Neuropharmacology Pub Date : 2025-04-30 DOI:10.1016/j.neuropharm.2025.110484

Luiz Felipe Souza e Silva , Amanda Siena , Jessica Mayumi Yuzawa , Tatiana Rosado Rosenstock

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引用次数: 0

Abstract

Hypoxia is a key environmental factor linked to neurodevelopmental complications, primarily through its impact on mitochondrial dysfunction. Given that sirtuins regulate mitochondrial and cellular metabolism, we aimed to investigate whether pharmacological modulation of sirtuins could protect neurons from hypoxia-induced mitochondrial dysfunction and cell death. To explore this, primary cortical neurons from male Wistar rats (control) and Spontaneously Hypertensive Rats (a model for neonatal hypoxia and schizophrenia) were exposed to cobalt chloride (CoCl₂) to chemically induce hypoxia. Neurons were also treated with Nicotinamide (50 μM), Resveratrol (0.5 μM), and Sirtinol (5 μM) to modulate sirtuin activity. We first assessed histone deacetylation, cell death, mitochondrial calcium retention capacity, mitochondrial membrane potential, and levels of reactive oxygen species (ROS). In addition, we analysed the expression of genes related to mitochondrial metabolism, dynamics, and biogenesis, as well as high-energy compound levels. Our data indicate that both chemical and neonatal hypoxia caused mitochondrial depolarization, reduced calcium retention, increased ROS levels, and elevated Nfe2l2 expression in primary cortical neurons. Hypoxia also led to increased expression of genes associated with mitochondrial biogenesis and fission, as well as reduced ATP levels and elevated pyruvate and lactate levels. Importantly, treatment with sirtuin modulators enhanced neuron viability, likely by further increasing Nfe2l2 expression and reducing ROS production. These modulators also improved metabolic outcomes, including higher ATP levels, and normalised pyruvate and lactate production, as well as mitochondrial fusion gene expression. Collectively, our findings suggest that sirtuin modulators could mitigate hypoxia-induced damage and may represent a potential therapeutic strategy for managing neurodevelopmental disorders.

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由于组蛋白3乙酰化和线粒体功能、动力学和含量的改变，Sirtuins调节剂减轻了缺氧诱导的细胞死亡

缺氧是与神经发育并发症相关的关键环境因素，主要通过其对线粒体功能障碍的影响。鉴于sirtuins调节线粒体和细胞代谢，我们旨在研究sirtuins的药理调节是否可以保护神经元免受缺氧诱导的线粒体功能障碍和细胞死亡。为了探讨这一点，将雄性Wistar大鼠（对照组）和自发性高血压大鼠（新生儿缺氧和精神分裂症模型）的初级皮质神经元暴露于氯化钴（CoCl2）中以化学方式诱导缺氧。同时，用烟酰胺（50 μM）、白藜芦醇（0.5 μM）和Sirtinol （5 μM）处理神经元，调节sirtuin活性。我们首先评估了组蛋白去乙酰化、细胞死亡、线粒体钙保留能力、线粒体膜电位和活性氧（ROS）水平。此外，我们分析了与线粒体代谢、动力学、生物发生以及高能化合物水平相关的基因表达。我们的数据表明，化学缺氧和新生儿缺氧都会导致线粒体去极化，钙潴留减少，ROS水平升高，初级皮质神经元中Nfe2l2表达升高。缺氧还导致与线粒体生物发生和裂变相关的基因表达增加，ATP水平降低，丙酮酸和乳酸水平升高。重要的是，用sirtuin调节剂治疗可能通过进一步增加Nfe2l2表达和减少ROS产生来增强神经元的活力。这些调节剂还改善了代谢结果，包括更高的ATP水平，正常化的丙酮酸和乳酸生成，以及线粒体融合基因表达。总的来说，我们的研究结果表明sirtuin调节剂可以减轻缺氧引起的损伤，并可能代表一种潜在的治疗神经发育障碍的策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Neuropharmacology 医学-神经科学

CiteScore

10.00

自引率

4.30%

发文量

288

审稿时长

45 days

期刊介绍： Neuropharmacology publishes high quality, original research and review articles within the discipline of neuroscience, especially articles with a neuropharmacological component. However, papers within any area of neuroscience will be considered. The journal does not usually accept clinical research, although preclinical neuropharmacological studies in humans may be considered. The journal only considers submissions in which the chemical structures and compositions of experimental agents are readily available in the literature or disclosed by the authors in the submitted manuscript. Only in exceptional circumstances will natural products be considered, and then only if the preparation is well defined by scientific means. Neuropharmacology publishes articles of any length (original research and reviews).