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含组织型纤溶酶原激活剂/绿色荧光蛋白杂交体的颗粒轴突运输的实时成像

Real-time imaging of the axonal transport of granules containing a tissue plasminogen activator/green fluorescent protein hybrid.

作者信息

Lochner J E, Kingma M, Kuhn S, Meliza C D, Cutler B, Scalettar B A

机构信息

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

出版信息

Mol Biol Cell. 1998 Sep;9(9):2463-76. doi: 10.1091/mbc.9.9.2463.

Abstract

A hybrid protein, tPA/GFP, consisting of rat tissue plasminogen activator (tPA) and green fluorescent protein (GFP) was expressed in PC12 cells and used to study the distribution, secretory behavior, and dynamics of secretory granules containing tPA in living cells with a neuronal phenotype. High-resolution images demonstrate that tPA/GFP has a growth cone-biased distribution in differentiated cells and that tPA/GFP is transported in granules of the regulated secretory pathway that colocalize with granules containing secretogranin II. Time-lapse images of secretion reveal that secretagogues induce substantial loss of cellular tPA/GFP fluorescence, most importantly from growth cones. Time-lapse images of the axonal transport of granules containing tPA/GFP reveal a surprising complexity to granule dynamics. Some granules undergo canonical fast axonal transport; others move somewhat more slowly, especially in highly fluorescent neurites. Most strikingly, granules traffic bidirectionally along neurites to an extent that depends on granule accumulation, and individual granules can reverse their direction of motion. The retrograde component of this bidirectional transport may help to maintain cellular homeostasis by transporting excess tPA/GFP back toward the cell body. The results presented here provide a novel view of the axonal transport of secretory granules. In addition, the results suggest that tPA is targeted for regulated secretion from growth cones of differentiated cells, strategically positioning tPA to degrade extracellular barriers or to activate other barrier-degrading proteases during axonal elongation.

摘要

一种由大鼠组织型纤溶酶原激活剂(tPA)和绿色荧光蛋白(GFP)组成的杂合蛋白tPA/GFP在PC12细胞中表达,并用于研究具有神经元表型的活细胞中含tPA的分泌颗粒的分布、分泌行为和动力学。高分辨率图像显示,tPA/GFP在分化细胞中具有偏向生长锥的分布,并且tPA/GFP在受调节分泌途径的颗粒中运输,这些颗粒与含分泌粒蛋白II的颗粒共定位。分泌的延时图像显示,促分泌剂会导致细胞内tPA/GFP荧光大量丧失,最重要的是从生长锥处丧失。含tPA/GFP的颗粒轴突运输的延时图像显示颗粒动力学具有惊人的复杂性。一些颗粒进行典型的快速轴突运输;其他颗粒移动稍慢,尤其是在高荧光神经突中。最引人注目的是,颗粒沿神经突双向运输,其程度取决于颗粒的积累,并且单个颗粒可以反转其运动方向。这种双向运输的逆行成分可能通过将过量的tPA/GFP运回细胞体来帮助维持细胞内稳态。此处呈现的结果提供了分泌颗粒轴突运输的新观点。此外,结果表明tPA靶向于分化细胞生长锥的调节性分泌,将tPA战略性地定位以在轴突伸长过程中降解细胞外屏障或激活其他降解屏障的蛋白酶。

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