Karolina Przepiórska-Drońska, Agnieszka Wnuk, Bernadeta Angelika Pietrzak-Wawrzyńska, Andrzej Łach, Weronika Biernat, Anna Katarzyna Wójtowicz, Małgorzata Kajta
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Post-treatment with amorfrutin B decreased the IBA1 fluorescence intensity, reduced caspase-1 activity, and downregulated IL1B/IL-1β and TNFA but not IL10/IL-10 expression, which was upregulated. Amorfrutin B also stimulated PPARγ signaling, as evidenced by increased mRNA and/or protein levels of PPARγ and PGC1α. In addition, amorfrutin B reversed the hypoxia/ischemia-evoked effects on mitochondria-related parameters, such as mitochondrial membrane potential, BCL2/BCL2 expression and metabolic activity, which were correlated with diminished proliferation potential of microglia. Interestingly, the inhibitory effect of amorfrutin B on the proliferation potential and mitochondrial function of microglia is opposite to the stimulatory effect of amorfrutin B on mouse neuronal survival, as evidenced by increased neuronal viability and reduced neurodegeneration. In summary, this study showed for the first time that amorfrutin B compromises hypoxia/ischemia-induced activation of human microglia in a PPARγ-dependent manner, which involves inhibiting inflammation, normalizing mitochondrial status, and controlling proliferation potential. These data extend the protective potential of amorfrutin B in the pharmacotherapy of hypoxic/ischemic brain injury, targeting not only neurons but also activated microglia.</p>","PeriodicalId":73858,"journal":{"name":"Journal of neuroimmune pharmacology : the official journal of the Society on NeuroImmune Pharmacology","volume":"19 1","pages":"34"},"PeriodicalIF":6.2000,"publicationDate":"2024-07-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11217078/pdf/","citationCount":"0","resultStr":"{\"title\":\"Amorfrutin B Compromises Hypoxia/Ischemia-induced Activation of Human Microglia in a PPARγ-dependent Manner: Effects on Inflammation, Proliferation Potential, and Mitochondrial Status.\",\"authors\":\"Karolina Przepiórska-Drońska, Agnieszka Wnuk, Bernadeta Angelika Pietrzak-Wawrzyńska, Andrzej Łach, Weronika Biernat, Anna Katarzyna Wójtowicz, Małgorzata Kajta\",\"doi\":\"10.1007/s11481-024-10135-9\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Amorfrutin B is a selective PPARγ modulator that we demonstrated to be a promising neuroprotective compound in cellular models of stroke and perinatal asphyxia. 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引用次数: 0
摘要
Amorfrutin B 是一种选择性 PPARγ 调节剂,我们在中风和围产期窒息的细胞模型中证明它是一种很有前途的神经保护化合物。虽然已经确定了amorfrutin B诱发神经保护的神经元机制,但它们都没有反映出该化合物对小胶质细胞的作用,而小胶质细胞在大脑对缺氧/缺血的反应中起着关键作用。在这里,我们提供了阿莫罗汀 B 对缺氧/缺血状态下的人类小胶质细胞产生作用的证据;该化合物能抵消炎症,并以 PPARγ 依赖性方式影响线粒体状态和增殖潜能。用amorfrutin B治疗后,IBA1荧光强度下降,caspase-1活性降低,IL1B/IL-1β和TNFA表达下调,但IL10/IL-10表达未见上调。阿莫鲁丁 B 还能刺激 PPARγ 信号传导,表现为 PPARγ 和 PGC1α 的 mRNA 和/或蛋白水平升高。此外,阿莫鲁丁 B 还逆转了缺氧/缺血对线粒体相关参数(如线粒体膜电位、BCL2/BCL2 表达和代谢活性)的影响,这些影响与小胶质细胞增殖潜力的减弱相关。有趣的是,阿莫鲁丁 B 对小胶质细胞增殖潜能和线粒体功能的抑制作用与阿莫鲁丁 B 对小鼠神经元存活的刺激作用相反,表现为神经元存活率的提高和神经变性的减少。总之,这项研究首次表明,阿莫鲁丁 B 能以 PPARγ 依赖性方式损害缺氧/缺血诱导的人小胶质细胞激活,其中包括抑制炎症、使线粒体状态正常化以及控制增殖潜能。这些数据拓展了阿莫罗汀 B 在缺氧/缺血性脑损伤药物治疗中的保护潜力,它不仅针对神经元,还针对活化的小胶质细胞。
Amorfrutin B Compromises Hypoxia/Ischemia-induced Activation of Human Microglia in a PPARγ-dependent Manner: Effects on Inflammation, Proliferation Potential, and Mitochondrial Status.
Amorfrutin B is a selective PPARγ modulator that we demonstrated to be a promising neuroprotective compound in cellular models of stroke and perinatal asphyxia. Although neuronal mechanisms of amorfrutin B-evoked neuroprotection have been identified, none of them reflects the actions of the compound on microglia, which play a pivotal role in brain response to hypoxia/ischemia. Here, we provide evidence for amorfrutin B-induced effects on human microglia subjected to hypoxia/ischemia; the compound counteracts inflammation, and influences mitochondrial status and proliferation potential in a PPARγ-dependent manner. Post-treatment with amorfrutin B decreased the IBA1 fluorescence intensity, reduced caspase-1 activity, and downregulated IL1B/IL-1β and TNFA but not IL10/IL-10 expression, which was upregulated. Amorfrutin B also stimulated PPARγ signaling, as evidenced by increased mRNA and/or protein levels of PPARγ and PGC1α. In addition, amorfrutin B reversed the hypoxia/ischemia-evoked effects on mitochondria-related parameters, such as mitochondrial membrane potential, BCL2/BCL2 expression and metabolic activity, which were correlated with diminished proliferation potential of microglia. Interestingly, the inhibitory effect of amorfrutin B on the proliferation potential and mitochondrial function of microglia is opposite to the stimulatory effect of amorfrutin B on mouse neuronal survival, as evidenced by increased neuronal viability and reduced neurodegeneration. In summary, this study showed for the first time that amorfrutin B compromises hypoxia/ischemia-induced activation of human microglia in a PPARγ-dependent manner, which involves inhibiting inflammation, normalizing mitochondrial status, and controlling proliferation potential. These data extend the protective potential of amorfrutin B in the pharmacotherapy of hypoxic/ischemic brain injury, targeting not only neurons but also activated microglia.
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