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从大鼠脑中纯化过氧化物酶体组分。

Purification of peroxisomal fraction from rat brain.

作者信息

Cimini A M, Moreno S, Giorgi M, Serafini B, Cerú M P

机构信息

Department of Science and Biomedical Technology, University of L'Aquila, Italy.

出版信息

Neurochem Int. 1993 Sep;23(3):249-60. doi: 10.1016/0197-0186(93)90116-m.

Abstract

A purification procedure to obtain peroxisomes (microperoxisomes) from the brain of suckling rats is reported. A P2 fraction, (crude light mitochondria) frozen and thawed seven times, was subfractionated yielding a P4 fraction, 4-fold enriched in catalase activity with respect to the cytoplasmic extract S1. The P4 fraction was used for further purification of peroxisomes by isopicnic centrifugation on Nycodenz gradient (1.10-1.20 g/ml). When the cerebellum was not included in the starting material, the equilibrium density of peroxisomes was 1.152-1.162 g/ml. In this case the overall yield of catalase in the most enriched fraction was 7% and its relative specific activity more than 50. When the cerebellum was included in the total homogenate, the equilibrium density shifted towards higher values (1.177 g/ml) and in this case the catalase relative specific activity in the peroxisomal enriched fraction was extremely high (> 100). The biochemical results, together with the electron microscope examination of the purified fractions, demonstrate that our procedure allows the best purification of brain peroxisomes so far obtained. The different equilibrium densities of peroxisomes observed in the two sets of experiments are interpreted in terms of size heterogeneity of these organelles in different brain portions and cell types.

摘要

本文报道了一种从乳鼠大脑中获取过氧化物酶体(微过氧化物酶体)的纯化方法。将经过七次冻融的P2组分(粗制轻线粒体)进行亚分级分离,得到P4组分,其过氧化氢酶活性相对于细胞质提取物S1富集了4倍。P4组分用于通过在Nycodenz梯度(1.10 - 1.20 g/ml)上进行等密度离心进一步纯化过氧化物酶体。当起始材料中不包含小脑时,过氧化物酶体的平衡密度为1.152 - 1.162 g/ml。在这种情况下,最富集组分中过氧化氢酶的总产率为7%,其相对比活性超过50。当总匀浆中包含小脑时,平衡密度向更高值(1.177 g/ml)移动,在这种情况下,过氧化物酶体富集组分中过氧化氢酶的相对比活性极高(> 100)。生化结果以及对纯化组分的电子显微镜检查表明,我们的方法能够实现迄今为止对脑过氧化物酶体的最佳纯化。两组实验中观察到的过氧化物酶体不同平衡密度,可根据这些细胞器在不同脑区和细胞类型中的大小异质性来解释。

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