首页> 外文期刊>Brain research >Regulation of phosphorylation of neuronal microtubule-associated proteins MAP1b and MAP2 by protein phosphatase-2A and -2B in rat brain.
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Regulation of phosphorylation of neuronal microtubule-associated proteins MAP1b and MAP2 by protein phosphatase-2A and -2B in rat brain.

机译:大鼠脑中蛋白质磷酸酶2A和-2B调节神经元微管相关蛋白MAP1b和MAP2的磷酸化。

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摘要

The function of the neuronal high molecular weight microtubule-associated proteins (MAPs) MAP1b and MAP2 is regulated by the degree of their phosphorylation, which in turn is controlled by the activities of protein kinases and protein phosphatases (PP). To investigate the role of PP in the regulation of the phosphorylation of MAP1b and MAP2, we used okadaic acid and cyclosporin A to selectively inhibit PP2A and PP2B activities, respectively, in metabolically competent rat brain slices. The alteration of the phosphorylation levels of MAP1b and MAP2 was examined by Western blots using several phosphorylation-dependent antibodies to these proteins. The inhibition of PP2A, and to a lesser extent of PP2B, was found to induce an increased phosphorylation of MAP1b and inhibit its microtubule binding activity. Immunocytochemically, a marked increase in neuronal staining in inhibitor-treated tissue was observed with antibodies to the phosphorylated MAP1b. The inhibition of PP2A but not of PP2B also induced phosphorylation of MAP2 at multiple sites and impaired its microtubule binding activity. These results suggest that PP2A might be the major PP that participates in regulation of the phosphorylation of MAP1b and MAP2 and their biological activities.
机译:神经元高分子量微管相关蛋白(MAPs)MAP1b和MAP2的功能受其磷酸化程度的调节,而磷酸化程度又受蛋白激酶和蛋白磷酸酶(PP)的活性控制。为了研究PP在调节MAP1b和MAP2磷酸化中的作用,我们使用了冈田酸和环孢菌素A分别选择性地抑制了具有代谢能力的大鼠脑切片中的PP2A和PP2B活性。 MAP1b和MAP2磷酸化水平的变化是通过Western blot检测的,这些蛋白使用了几种依赖于这些蛋白质的磷酸化依赖性抗体。发现抑制PP2A和程度较小的PP2B可以诱导MAP1b磷酸化增加,并抑制其微管结合活性。免疫细胞化学法观察到,用磷酸化的MAP1b抗体可抑制抑制剂处理的组织中神经元染色的明显增加。对PP2A的抑制而不是对PP2B的抑制也诱导了MAP2在多个位点的磷酸化,并削弱了其微管结合活性。这些结果表明,PP2A可能是参与MAP1b和MAP2磷酸化及其生物学活性调控的主要PP。

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