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ReMAPping the microtubule landscape: How phosphorylation dictates the activities of microtubule‐associated proteins

机译:重新唤起微管景观:磷酸化如何决定微管相关蛋白的活性

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Classical microtubule‐associated proteins (MAPs) were originally identified based on their co‐purification with microtubules assembled from mammalian brain lysate. They have since been found to perform a range of functions involved in regulating the dynamics of the microtubule cytoskeleton. Most of these MAPs play integral roles in microtubule organization during neuronal development, microtubule remodeling during neuronal activity, and microtubule stabilization during neuronal maintenance. As a result, mutations in MAPs contribute to neurodevelopmental disorders, psychiatric conditions, and neurodegenerative diseases. MAPs are post‐translationally regulated by phosphorylation depending on developmental time point and cellular context. Phosphorylation can affect the microtubule affinity, cellular localization, or overall function of a particular MAP and can thus have profound implications for neuronal health. Here we review MAP1, MAP2, MAP4, MAP6, MAP7, MAP9, tau, and DCX, and how each is regulated by phosphorylation in neuronal physiology and disease. Developmental Dynamics 247:138–155, 2018 . ? 2017 Wiley Periodicals, Inc.
机译:典型的微管相关蛋白(MAPS)最初是基于它们的纯化与哺乳动物脑裂解物组装的微管纯化来鉴定。由于已被发现执行一系列涉及调节微管细胞骨架的动态的功能。这些地图中的大多数在神经元发育期间在微管组织中发挥不良作用,神经元活动期间的微管重塑,以及神经元维持期间的微管稳定。结果,地图中的突变有助于神经发育障碍,精神病病症和神经变性疾病。根据发育时间点和蜂窝环境,地图是通过磷酸化的翻译后调节。磷酸化可以影响特定地图的微管亲和力,细胞定位或整体功能,因此可以对神经元健康产生深远的影响。在这里,我们审查Map1,Map2,Map4,Map6,Map7,Map9,Tau和DCX,以及如何通过神经元生理和疾病中的磷酸化进行调节。发展动力学247:138-155,2018。还2017年Wiley期刊,Inc。

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