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SNAP可防止Mg(2+)-ATP诱导的N-乙基马来酰亚胺敏感因子从洋地黄皂苷通透的PC12细胞的高尔基体释放。

SNAP prevents Mg(2+)-ATP-induced release of N-ethylmaleimide-sensitive factor from the Golgi apparatus in digitonin-permeabilized PC12 cells.

作者信息

Tagaya M, Furuno A, Mizushima S

机构信息

School of Life Science, Tokyo University of Pharmacy and Life Science, Japan.

出版信息

J Biol Chem. 1996 Jan 5;271(1):466-70. doi: 10.1074/jbc.271.1.466.

Abstract

The N-ethylmaleimide-sensitive factor (NSF), which is involved in the multisteps of protein transport, is released from Golgi membranes on in vitro incubation with Mg(2+)-ATP. However, several lines of evidence suggest that NSF is associated with membranes in spite of the presence of Mg2+ and ATP in vivo. We have used digitonin-permeabilized PC12 cells to investigate the mechanism underlying the association of NSF with membranes. In PC12 cells, immunoreactivity for NSF was observed in the nuclear membranes, the Golgi apparatus, and neuronal growth cones, where synaptic vesicles are concentrated. NSF associated with the Golgi apparatus was released on incubation with Mg(2+)-ATP, whereas NSF in the nuclear membranes and neuronal growth cones was not released on the same treatment. The addition of cytosol blocked the Mg(2+)-ATP-induced release of NSF from the Golgi apparatus. Chromatographic analyses revealed that the factor(s) that prevents NSF release from the Golgi apparatus was eluted at the same position as the soluble NSF attachment proteins (SNAPs). Purified His6-tagged alpha-SNAP exhibited such activity. His6-tagged alpha-SNAP also prevented the Mg(2+)-ATP-induced release of NSF from isolated Golgi membranes.

摘要

参与蛋白质运输多个步骤的N - 乙基马来酰亚胺敏感因子(NSF),在与Mg(2 +)-ATP进行体外孵育时会从高尔基体膜上释放出来。然而,几条证据表明,尽管体内存在Mg2 +和ATP,但NSF仍与膜相关联。我们使用洋地黄皂苷通透的PC12细胞来研究NSF与膜相关联的潜在机制。在PC12细胞中,在核膜、高尔基体和神经元生长锥中观察到了NSF的免疫反应性,而突触小泡集中在这些部位。与高尔基体相关联的NSF在与Mg(2 +)-ATP孵育时会释放出来,而核膜和神经元生长锥中的NSF在相同处理下不会释放。添加胞质溶胶可阻止Mg(2 +)-ATP诱导的NSF从高尔基体释放。色谱分析表明,阻止NSF从高尔基体释放的因子在与可溶性NSF附着蛋白(SNAPs)相同的位置被洗脱。纯化的His6标记的α-SNAP表现出这种活性。His6标记的α-SNAP也阻止了Mg(2 +)-ATP诱导的NSF从分离的高尔基体膜上释放。

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