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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Biochemical pathways by which serotonin regulates translation in the nervous system of Aplysia.
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Biochemical pathways by which serotonin regulates translation in the nervous system of Aplysia.

机译:血清素调节海藻神经系统翻译的生化途径。

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In the marine mollusk Aplysia californica, serotonin initiates three phases of translational regulation: an initial decrease in translation, followed by a transient increase in protein synthesis, both of which are independent of transcription, followed by a later increase in protein synthesis that is dependent on transcription. These increases in protein synthesis may underlie translation-dependent changes in synaptic plasticity. We have characterized the second messenger pathways that underlie these changes in the pleural ganglia of Aplysia. Activation of protein kinase C was both necessary and sufficient for the initial decrease in translation. Protein kinase C, cyclic AMP-dependent protein kinase, and a tyrosine kinase were all required for the second phase, a transient increase in protein synthesis. The late increase in protein synthesis required both protein kinase A and spaced applications of serotonin. Rapamycin, a specific inhibitor of a downstream translational regulator, blocked the transient increase in protein synthesis (second phase), suggesting that this drug may be useful in determining the specific physiological consequences of this translational regulation. Indeed, we used rapamycin to demonstrate that one type of intermediate form of synaptic plasticity induced by serotonin did not require the rapamycin-sensitive increase in translation.
机译:在海洋软体动物Aplysia californica中,5-羟色胺启动了翻译调节的三个阶段:翻译的初始降低,随后是蛋白质合成的短暂增加,这两者均与转录无关,然后是依赖于蛋白质合成的后来增加。转录。蛋白质合成的这些增加可能是突触可塑性的翻译依赖性变化的基础。我们已经表征了第二信使通路,这些通路是海藻胸膜神经节中这些变化的基础。蛋白激酶C的激活对于翻译的最初减少既必要又充分。第二阶段都需要蛋白激酶C,环状AMP依赖性蛋白激酶和酪氨酸激酶,这是蛋白合成的短暂增加。蛋白质合成的后期增加需要蛋白质激酶A和5-羟色胺的间隔应用。雷帕霉素是下游翻译调节剂的特异性抑制剂,它阻止了蛋白质合成的瞬时增加(第二阶段),这表明该药物可用于确定这种翻译调节的特定生理后果。确实,我们使用雷帕霉素来证明由5-羟色胺诱导的一种中间形式的突触可塑性并不要求雷帕霉素敏感的翻译增加。

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