Department of Life Sciences, National Chung Hsing University, Taichung, Taiwan.
Department of Medical Research, Translational Cell Therapy Center, China Medical University Hospital, Taichung, Taiwan.
Am J Physiol Cell Physiol. 2024 Jun 1;326(6):C1648-C1658. doi: 10.1152/ajpcell.00121.2024. Epub 2024 Apr 29.
The authors' previous research has shown the pivotal roles of cyclin-dependent kinase 5 (CDK5) and its regulatory protein p35 in nerve growth factor (NGF)-induced differentiation of sympathetic neurons in PC12 cells. During the process of differentiation, neurons are susceptible to environmental influences, including the effects of drugs. Metformin is commonly used in the treatment of diabetes and its associated symptoms, particularly in diabetic neuropathy, which is characterized by dysregulation of the sympathetic neurons. However, the impacts of metformin on sympathetic neuronal differentiation remain unknown. In this study, we investigated the impact of metformin on NGF-induced sympathetic neuronal differentiation using rat pheochromocytoma PC12 cells as a model. We examined the regulation of TrkA-p35/CDK5 signaling in NGF-induced PC12 differentiation. Our results demonstrate that metformin reduces NGF-induced PC12 differentiation by inactivating the TrkA receptor, subsequently inhibiting ERK and EGR1. Inhibition of this cascade ultimately leads to the downregulation of p35/CDK5 in PC12 cells. Furthermore, metformin inhibits the activation of the presynaptic protein Synapsin-I, a substrate of CDK5, in PC12 differentiation. In addition, metformin alters axonal and synaptic bouton formation by inhibiting p35 at both the axons and axon terminals in fully differentiated PC12 cells. In summary, our study elucidates that metformin inhibits sympathetic neuronal differentiation in PC12 cells by disrupting TrkA/ERK/EGR1 and p35/CDK5 signaling. This research contributes to uncovering a novel signaling mechanism in drug response during sympathetic neuronal differentiation, enhancing our understanding of the intricate molecular processes governing this critical aspect of neurodevelopment. This study unveils a novel mechanism influenced by metformin during sympathetic neuronal differentiation. By elucidating its inhibitory effects from the nerve growth factor (NGF) receptor, TrkA, to the p35/CDK5 signaling pathways, we advance our understanding of metformin's mechanisms of action and emphasize its potential significance in the context of drug responses during sympathetic neuronal differentiation.
作者之前的研究表明,细胞周期蛋白依赖性激酶 5(CDK5)及其调节蛋白 p35 在神经生长因子(NGF)诱导 PC12 细胞交感神经元分化中起着关键作用。在分化过程中,神经元易受环境影响,包括药物的影响。二甲双胍常用于治疗糖尿病及其相关症状,特别是在糖尿病性神经病变中,其特征是交感神经元失调。然而,二甲双胍对交感神经元分化的影响尚不清楚。在这项研究中,我们使用大鼠嗜铬细胞瘤 PC12 细胞作为模型,研究了二甲双胍对 NGF 诱导的交感神经元分化的影响。我们研究了 NGF 诱导的 PC12 分化中 TrkA-p35/CDK5 信号的调节。研究结果表明,二甲双胍通过使 TrkA 受体失活来减少 NGF 诱导的 PC12 分化,进而抑制 ERK 和 EGR1。该级联反应的抑制最终导致 PC12 细胞中 p35/CDK5 的下调。此外,二甲双胍抑制 CDK5 的底物突触小体蛋白 Synapsin-I 在 PC12 分化中的激活。此外,二甲双胍通过抑制完全分化的 PC12 细胞中的轴突和轴突末端的 p35 来改变轴突和突触小泡的形成。总之,我们的研究表明,二甲双胍通过破坏 TrkA/ERK/EGR1 和 p35/CDK5 信号来抑制 PC12 细胞中的交感神经元分化。这项研究揭示了交感神经元分化过程中药物反应的新信号机制,增强了我们对调控神经发育这一关键方面的复杂分子过程的理解。这项研究揭示了二甲双胍在交感神经元分化过程中受到影响的新机制。通过阐明其从神经生长因子(NGF)受体 TrkA 到 p35/CDK5 信号通路的抑制作用,我们加深了对二甲双胍作用机制的理解,并强调了其在交感神经元分化过程中药物反应中的潜在意义。
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