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一种直接从S1组分中分离突触体的快速Percoll梯度离心法:亚细胞组分的活力

A rapid Percoll gradient procedure for isolation of synaptosomes directly from an S1 fraction: viability of subcellular fractions.

作者信息

Harrison S M, Jarvie P E, Dunkley P R

机构信息

Neuroscience Group, Faculty of Medicine, University of Newcastle, New South Wales, Australia.

出版信息

Brain Res. 1988 Feb 16;441(1-2):72-80. doi: 10.1016/0006-8993(88)91384-4.

Abstract

The metabolic and functional viability of synaptosomes was examined in 5 subcellular fractions obtained after centrifugation of an S1 fraction from rat cerebral cortex on a discontinuous Percoll gradient (Brain Research, this volume, 1987). Fraction 4 was the most enriched for viable synaptosomes since, although it accounted for only 11.8% of the total protein recovered from the gradient, this fraction contained 23.7% of the basal synapsin I phosphorylation activity, the greatest degree of depolarisation-stimulated increase in synapsin I phosphorylation, 36.1% of the total [3H]noradrenaline uptake capacity and 46.9% of the total [3H]noradrenaline release capacity. Noradrenaline release from fraction 4 was consistent with a neuronal mechanism as it was increased with increasing K+ concentrations and was dependent on calcium. Fractions 1 and 2 contained few viable synaptosomes as judged by their capacity for noradrenaline uptake and release, yet these fractions accounted for some 62.6% of the endogenous content of noradrenaline. In part their lack of viability was due to a low content of intrasynaptosomal mitochondria, while their high content of endogenous noradrenaline was due to the presence of synaptic vesicles released from damaged nerve terminals. The synaptosomes in fraction 3 were metabolically and functionally viable, but their capacity for uptake and release of noradrenaline was lower than for fraction 4. The synaptosomes in fraction 5 showed only a small depolarisation-stimulated release of noradrenaline, suggesting a lack of viability. Part of the capacity for uptake of [3H]noradrenaline into fraction 5 was attributed to the presence of extrasynaptosomal mitochondria.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在通过对大鼠大脑皮层的S1组分在不连续Percoll梯度上进行离心获得的5个亚细胞组分中,检测了突触体的代谢和功能活性(《脑研究》,本期,1987年)。组分4富含活性突触体,因为尽管它仅占从梯度中回收的总蛋白的11.8%,但该组分含有23.7%的基础突触素I磷酸化活性、最大程度的去极化刺激的突触素I磷酸化增加、36.1%的总[3H]去甲肾上腺素摄取能力和46.9%的总[3H]去甲肾上腺素释放能力。组分4中的去甲肾上腺素释放符合神经元机制,因为它随着钾离子浓度的增加而增加,并且依赖于钙。根据其去甲肾上腺素摄取和释放能力判断,组分1和2含有很少的活性突触体,但这些组分占去甲肾上腺素内源性含量的约62.6%。它们缺乏活性部分是由于突触体内线粒体含量低,而其高含量的内源性去甲肾上腺素是由于受损神经末梢释放的突触小泡的存在。组分3中的突触体在代谢和功能上是有活性的,但其去甲肾上腺素摄取和释放能力低于组分4。组分5中的突触体仅显示出小的去极化刺激的去甲肾上腺素释放,表明缺乏活性。[3H]去甲肾上腺素摄取到组分5中的部分能力归因于突触体外线粒体的存在。(摘要截短于250字)

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