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磷酸化微管相关蛋白tau在发育中的皮质神经元中的分布。

Distribution of the phosphorylated microtubule-associated protein tau in developing cortical neurons.

作者信息

Brion J P, Octave J N, Couck A M

机构信息

Laboratory of Pathology and Electron Microscopy, Université Libre de Bruxelles, Belgium.

出版信息

Neuroscience. 1994 Dec;63(3):895-909. doi: 10.1016/0306-4522(94)90533-9.

Abstract

During brain development, the microtubule-associated protein tau presents a transient state of high phosphorylation. We have investigated the developmental distribution of the phosphorylated fetal-type tau in the developing rat cortex and in cultures of embryonic cortical neurons, using antibodies which react with tau in a phosphorylation-dependent manner. The phosphorylated fetal-type tau was present in the developing cortex at 20 days but not at 18 days of embryonic life and was not detected before four to five days in neuronal culture. The cyclin-dependent kinase p34cdc2 was expressed only in germinal layers in the embryonic brain and was not co-localized with phosphorylated tau. After 10 days of postnatal life, the phosphorylated tau progressively disappeared from cortical neurons, disappearing first from the deepest cortical layers where neurons are ontogenetically the oldest. Phosphorylated tau was found in axons and dendrites of cortical neurons at all developmental stages whereas unphosphorylated tau tended to disappear from dendrites during development. The timing of appearance of phosphorylated tau in the cortex, by comparison with the expression of other developmental markers, indicates that phosphorylated tau is present at a high level only during the period of intense neuritic outgrowth and that it disappears during the period of neurite stabilization and synaptogenesis, concomitantly to the expression of adult tau isoforms. In control cultures and in cultures treated with colchicine, the phosphorylated tau was not associated to cold-stable and to colchicine-resistant microtubules. These in vivo results suggest that the high expression of phosphorylated tau species is correlated with the presence of a dynamic microtubule network during a period of high plasticity in the developing brain.

摘要

在大脑发育过程中,微管相关蛋白tau呈现出高磷酸化的短暂状态。我们使用以磷酸化依赖性方式与tau反应的抗体,研究了磷酸化胎儿型tau在发育中的大鼠皮质和胚胎皮质神经元培养物中的发育分布。磷酸化胎儿型tau在胚胎期20天的发育中的皮质中存在,但在胚胎期18天不存在,并且在神经元培养四到五天之前未检测到。细胞周期蛋白依赖性激酶p34cdc2仅在胚胎脑的生发层中表达,并且不与磷酸化tau共定位。出生后10天,磷酸化tau从皮质神经元中逐渐消失,首先从皮质最深层消失,这些层的神经元在个体发育上是最古老的。在所有发育阶段,磷酸化tau存在于皮质神经元的轴突和树突中,而未磷酸化的tau在发育过程中倾向于从树突中消失。与其他发育标志物的表达相比,皮质中磷酸化tau出现的时间表明,磷酸化tau仅在强烈的神经突生长期间高水平存在,并且在神经突稳定和突触形成期间消失,同时伴随着成人tau异构体的表达。在对照培养物和用秋水仙碱处理的培养物中,磷酸化tau与冷稳定和秋水仙碱抗性微管无关。这些体内结果表明,磷酸化tau物种的高表达与发育中的大脑高可塑性期间动态微管网络的存在相关。

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