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J Neurosci. 1982 Aug;2(8):1157-75. doi: 10.1523/JNEUROSCI.02-08-01157.1982.
2
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PC12细胞的神经突生长和蛋白质合成与底物及神经生长因子的关系。

Neurite outgrowth and protein synthesis by PC12 cells as a function of substratum and nerve growth factor.

作者信息

Fujii D K, Massoglia S L, Savion N, Gospodarowicz D

出版信息

J Neurosci. 1982 Aug;2(8):1157-75. doi: 10.1523/JNEUROSCI.02-08-01157.1982.

DOI:10.1523/JNEUROSCI.02-08-01157.1982
PMID:7108587
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6564279/
Abstract

Numerous studies have implied that enhanced cell-substratum adhesion plays a role in neurite outgrowth by neuronal cells. Using an extracellular matrix (ECM) produced by cultured corneal endothelial cells, we have investigated attachment and de novo neurite outgrowth by the pheochromocytoma cell line, PC12. PC12 cells were found to attach more rapidly and efficiently to the ECM than to plastic or collagen-coated surfaces. An extensive but temporary (5- to 10-day) neurite outgrowth occurred in the absence of nerve growth factor (NGF) when cells were on the ECM. However, long term neurite survival and further elongation required NGF. Our findings are consistent with the hypothesis that protein(s) in the ECM has an important role in neurite outgrowth. Thus, NGF may not so much initiate neurite outgrowth as it stabilizes neurites. ECM and NGF also were found to modulate cellular protein synthesis by PC12 cells. On ECM, a decreased synthesis of many high molecular weight proteins (Mr greater than 85,000) was observed in comparison to that of cells on collagen-coated dishes. The presence of neurites (in the presence of absence of NGF) as associated with the induction of the synthesis of a cellular protein (Mr = 55,000 to 56,000 and pI of 5.6). NGF was found to increase markedly the synthesis of two secreted proteins, while it drastically reduced the synthesis of all others regardless of the substratum upon which the cells were maintained.

摘要

大量研究表明,增强的细胞与基质粘附在神经元细胞的神经突生长中起作用。利用培养的角膜内皮细胞产生的细胞外基质(ECM),我们研究了嗜铬细胞瘤细胞系PC12的附着和新生神经突生长情况。发现PC12细胞与ECM的附着比与塑料或胶原包被表面的附着更快且更有效。当细胞置于ECM上时,在没有神经生长因子(NGF)的情况下会发生广泛但短暂的(5至10天)神经突生长。然而,神经突的长期存活和进一步伸长需要NGF。我们的发现与ECM中的蛋白质在神经突生长中起重要作用这一假设一致。因此,NGF与其说是启动神经突生长,不如说是稳定神经突。还发现ECM和NGF可调节PC12细胞的细胞蛋白质合成。与胶原包被培养皿上的细胞相比,在ECM上观察到许多高分子量蛋白质(分子量大于85,000)的合成减少。神经突的存在(无论有无NGF)与一种细胞蛋白质(分子量为55,000至56,000,等电点为5.6)的合成诱导有关。发现NGF可显著增加两种分泌蛋白的合成,而无论细胞维持在何种基质上,它都会大幅降低所有其他蛋白的合成。