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活细胞成像揭示海马神经元树突棘中组织型纤溶酶原激活物的活性依赖性释放。

Activity-dependent release of tissue plasminogen activator from the dendritic spines of hippocampal neurons revealed by live-cell imaging.

作者信息

Lochner Janis E, Honigman Leah S, Grant Wilmon F, Gessford Sarah K, Hansen Alexis B, Silverman Michael A, Scalettar Bethe A

机构信息

Department of Chemistry, Lewis & Clark College, Portland, OR 97219, USA.

出版信息

J Neurobiol. 2006 May;66(6):564-77. doi: 10.1002/neu.20250.

DOI:10.1002/neu.20250
PMID:16555239
Abstract

Tissue plasminogen activator (tPA) has been implicated in a variety of important cellular functions, including learning-related synaptic plasticity and potentiating N-methyl-D-aspartate (NMDA) receptor-dependent signaling. These findings suggest that tPA may localize to, and undergo activity-dependent secretion from, synapses; however, conclusive data supporting these hypotheses have remained elusive. To elucidate these issues, we studied the distribution, dynamics, and depolarization-induced secretion of tPA in hippocampal neurons, using fluorescent chimeras of tPA. We found that tPA resides in dense-core granules (DCGs) that traffic to postsynaptic dendritic spines and that can remain in spines for extended periods. We also found that depolarization induced by high potassium levels elicits a slow, partial exocytotic release of tPA from DCGs in spines that is dependent on extracellular Ca(+2) concentrations. This slow, partial release demonstrates that exocytosis occurs via a mechanism, such as fuse-pinch-linger, that allows partial release and reuse of DCG cargo and suggests a mechanism that hippocampal neurons may rely upon to avoid depleting tPA at active synapses. Our results also demonstrate release of tPA at a site that facilitates interaction with NMDA-type glutamate receptors, and they provide direct confirmation of fundamental hypotheses about tPA localization and release that bear on its neuromodulatory functions, for example, in learning and memory.

摘要

组织型纤溶酶原激活剂(tPA)参与了多种重要的细胞功能,包括与学习相关的突触可塑性以及增强N-甲基-D-天冬氨酸(NMDA)受体依赖性信号传导。这些发现表明,tPA可能定位于突触,并从突触进行活性依赖性分泌;然而,支持这些假设的确凿数据仍然难以获得。为了阐明这些问题,我们使用tPA的荧光嵌合体研究了海马神经元中tPA的分布、动态变化以及去极化诱导的分泌。我们发现,tPA存在于致密核心囊泡(DCG)中,这些囊泡运输到突触后树突棘,并可在棘中长时间停留。我们还发现,高钾水平诱导的去极化会引发tPA从棘中的DCG缓慢、部分胞吐释放,这种释放依赖于细胞外Ca(+2)浓度。这种缓慢、部分释放表明,胞吐作用是通过一种机制发生的,比如融合-挤压-停留,这种机制允许DCG货物的部分释放和再利用,并提示了一种海马神经元可能依赖的机制,以避免在活跃突触处耗尽tPA。我们的结果还证明了tPA在一个便于与NMDA型谷氨酸受体相互作用的位点释放,并且它们直接证实了关于tPA定位和释放的基本假设,这些假设涉及其神经调节功能,例如在学习和记忆方面。

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