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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >A large-scale chemical screen for regulators of the arginase 1 promoter identifies the soy isoflavone daidzeinas a clinically approved small molecule that can promote neuronal protection or regeneration via a cAMP-independent pathway.
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A large-scale chemical screen for regulators of the arginase 1 promoter identifies the soy isoflavone daidzeinas a clinically approved small molecule that can promote neuronal protection or regeneration via a cAMP-independent pathway.

机译:氨基酶1启动子的调节剂的大规模化学筛网识别大豆异黄酮Daidzeinas临床批准的小分子,可通过营地无关的途径促进神经元保护或再生。

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摘要

An ideal therapeutic for stroke or spinal cord injury should promote survival and regeneration in the CNS. Arginase 1 (Arg1) has been shown to protect motor neurons from trophic factor deprivation and allow sensory neurons to overcome neurite outgrowth inhibition by myelin proteins. To identify small molecules that capture Arg1's protective and regenerative properties, we screened a hippocampal cell line stably expressing the proximal promoter region of the arginase 1 gene fused to a reporter gene against a library of compounds containing clinically approved drugs. This screen identified daidzein as a transcriptional inducer of Arg1. Both CNS and PNS neurons primed in vitro with daidzein overcame neurite outgrowth inhibition from myelin-associated glycoprotein, which was mirrored by acutely dissociated and cultured sensory neurons primed in vivo by intrathecal or subcutaneous daidzein infusion. Further, daidzein was effective in promoting axonal regeneration in vivo in an optic nerve crush model when given intraocularly without lens damage, or most importantly, when given subcutaneously after injury. Mechanistically, daidzein requires transcription and induction of Arg1 activity for its ability to overcome myelin inhibition. In contrast to canonical Arg1 activators, daidzein increases Arg1 without increasing CREB phosphorylation, suggesting its effects are cAMP-independent. Accordingly, it may circumvent known CNS side effects of some cAMP modulators. Indeed, daidzein appears to be safe as it has been widely consumed in soy products, crosses the blood-brain barrier, and is effective without pretreatment, making it an ideal candidate for development as a therapeutic for spinal cord injury or stroke.
机译:卒中或脊髓损伤的理想治疗性应促进CNS中的存活率和再生。已证明氨基酶1(Arc1)以保护来自营养因子剥夺的运动神经元,并且允许感觉神经元克服髓鞘蛋白的神经突血液抑制。为了鉴定捕获Arg1的保护和再生性质的小分子,我们筛选了稳定地表达融合在含有临床批准的药物的化合物文库中的邻接酶1基因的近端启动子区域的海马细胞系。该屏幕将Daidzein识别为Arg1的转录诱导剂。通过米隆相关糖蛋白的Daidzein克服神经蛋白生长抑制来自髓鞘和培养的感觉神经元,通过鞘内或皮下脱发,通过鞘内或皮下甲基蛋白的致染色和培养的感觉神经元映射的骨髓生物蛋白质过度抑制抑制的两种CNS和PNS神经元。此外,当损伤后,在眼内损伤或最重要的情况下,Daidzein促进在视神经挤压模型中促进体内体内的轴突再生促进轴突再生。机械地,Daidzeinin需要转录和诱导Arg1活动的克服髓鞘抑制的能力。与典型arg1激活剂相反,Daidzein增加了Arg1而​​不增加Creb磷酸化,表明其效果是无关的。因此,它可能是一些CAMP调制器的已知CNS副作用。事实上,大德尼州似乎是安全的,因为它在大豆产品中被广泛消耗,穿过血脑屏障,而没有预处理是有效的,使其成为脊髓损伤或中风治疗的理想候选者。

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