首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Critical role of TRPC1 in thyroid hormone-dependent dopaminergic neuron development
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Critical role of TRPC1 in thyroid hormone-dependent dopaminergic neuron development

机译:TRPC1在甲状腺激素依赖多巴胺能神经元发育中的关键作用

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Abstract Thyroid hormones play a crucial role in midbrain dopaminergic (DA) neuron development. However, the underlying molecular mechanisms remain largely unknown. In this study, we revealed that thyroid hormone treatment evokes significant calcium entry through canonical transient receptor potential (TRPC) channels in ventral midbrain neural stem cells and this calcium signaling is essential for thyroid hormone-dependent DA neuronal differentiation. We also found that TRPC1 is the dominant TRPC channel expressed in ventral midbrain neural stem cells which responds to thyroid hormone. In addition, thyroid hormone increases TRPC1 expression through its receptor alpha 1 during DA neuron differentiation, and, importantly, produces calcium signals by activating TRPC1 channels. In vivo and in vitro gene silencing experiments indicate that TRPC1-mediated calcium signaling is required for thyroid hormone-dependent DA neuronal differentiation. Finally, we confirmed that the activation of OTX2, a determinant of DA neuron development and the expression of which is induced by thyroid hormone, is dependent on TRPC1-mediated calcium signaling. These data revealed the molecular mechanisms of how thyroid hormone regulates DA neuron development from ventral midbrain neural stem cells, particularly endowing a novel physiological relevance to TRPC1 channels. Highlights ? Thyroid hormone evokes significant calcium entry in VM NSCs through TRPC1 channels. ? The expression of TRPC1 is dependent on thyroid hormone and TRα1. ? TRPC1-mediated calcium signaling is essential for thyroid hormone-dependent DA neuronal differentiation. ]]>
机译:摘要甲状腺激素在中脑多巴胺能(DA)神经元发育中发挥着至关重要的作用。然而,潜在的分子机制仍然很大程度上是未知的。在这项研究中,我们透露甲状腺激素治疗通过腹侧中脑神经干细胞中的规范瞬时受体电位(TRPC)通道唤起显着的钙进入,并且该钙信号对甲状腺激素依赖性DA神经元分化是必不可少的。我们还发现TRPC1是在腹侧中脑神经干细胞中表达的显性TRPC通道,其响应甲状腺激素。此外,甲状腺激素通过其受体α1期间通过其在DA神经元分化期间增加TRPC1表达,并且重要的是通过激活TRPC1通道产生钙信号。体内和体外基因沉默实验表明,TRPC1介导的钙信号传导是甲状腺激素依赖性DA神经元分化所必需的。最后,我们证实,OTX2的激活,DA神经元发育的决定因素以及甲状腺激素诱导的表达,取决于TRPC1介导的钙信号传导。这些数据揭示了甲状腺激素如何从腹侧中脑神经干细胞调节Da神经元发育的分子机制,特别是赋予与TRPC1通道的新的生理相关性。强调 ?甲状腺激素通过TRPC1通道唤起VM NSC的显着钙入口。还TRPC1的表达取决于甲状腺激素和TRα1。还TRPC1介导的钙信令对于甲状腺激素依赖性DA神经元分化至关重要。 ]]>

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