首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Protein kinase C activity regulates D-serine availability in the brain.
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Protein kinase C activity regulates D-serine availability in the brain.

机译:蛋白激酶C的活性调节大脑中D丝氨酸的利用率。

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摘要

D-serine is a co-agonist of NMDA receptor (NMDAR) and plays important roles in synaptic plasticity mechanisms. Serine racemase (SR) is a brain-enriched enzyme that converts L-serine to D-serine. SR interacts with the protein interacting with C-kinase 1 (PICK1), which is known to direct protein kinase C (PKC) to its targets in cells. Here, we investigated whether PKC activity regulates SR activity and D-serine availability in the brain. In vitro, PKC phosphorylated SR and decreased its activity. PKC activation increased SR phosphorylation in serine residues and reduced D-serine levels in astrocyte and neuronal cultures. Conversely, PKC inhibition decreased basal SR phosphorylation and increased cellular D-serine levels. In vivo modulation of PKC activity regulated both SR phosphorylation and D-serine levels in rat frontal cortex. Finally, rats that completed an object recognition task showed decreased SR phosphorylation and increased D-serine/total serine ratios, which was markedly correlated with decreased PKC activity in both cortex and hippocampus. Results indicate that PKC phosphorylates SR in serine residues and regulates D-serine availability in the brain. This interaction may be relevant for the regulation of physiological and pathological mechanisms linked to NMDAR function.
机译:D-丝氨酸是NMDA受体(NMDAR)的共激动剂,在突触可塑性机制中起重要作用。丝氨酸消旋酶(SR)是一种富含脑的酶,可将L-丝氨酸转化为D-丝氨酸。 SR与与C激酶1(PICK1)相互作用的蛋白质相互作用,该蛋白质已知将蛋白激酶C(PKC)引导至细胞中的靶标。在这里,我们调查了PKC活性是否调节大脑中SR活性和D-丝氨酸的利用率。在体外,PKC磷酸化SR,并降低其活性。 PKC激活增加星形胶质细胞和神经元培养物中丝氨酸残基的SR磷酸化,并降低D-丝氨酸水平。相反,PKC抑制可降低基础SR磷酸化并增加细胞D-丝氨酸水平。体内PKC活性的调节调节大鼠额叶皮层SR磷酸化和D丝氨酸水平。最后,完成对象识别任务的大鼠显示出SR磷酸化降低和D-丝氨酸/总丝氨酸比增加,这与皮层和海马中PKC活性降低显着相关。结果表明,PKC使丝氨酸残基中的SR磷酸化,并调节大脑中D-丝氨酸的利用率。这种相互作用可能与调节与NMDAR功能有关的生理和病理机制有关。

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