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葡萄球菌肠毒素B的转运与加工

Transport and processing of staphylococcal enterotoxin B.

作者信息

Tweten R K, Iandolo J J

出版信息

J Bacteriol. 1983 Jan;153(1):297-303. doi: 10.1128/jb.153.1.297-303.1983.

Abstract

A larger, membrane-bound form of staphylococcal enterotoxin B was shown by in vivo pulse-chase analysis to be the kinetic precursor to extracellular enterotoxin B. Processing of the enterotoxin B precursor molecules can apparently occur either cotranslationally or posttranslationally. Subcellular fractionation of cells revealed that all of the precursor toxin was associated with the membrane fraction. Once processed and released from the membrane, it was transiently associated with the cell wall before being released into the extracellular environment. The cell-wall-associated enterotoxin B was completely resistant to protease treatment and to extraction by high- or low-salt solutions at 0 to 2 degrees C, although it could be easily released from the cell by removal of the cell wall with lysostaphin. These data imply that newly formed enterotoxin B may be temporarily sequestered in specialized regions that require cell wall integrity before being released into the extracellular environment.

摘要

体内脉冲追踪分析表明,葡萄球菌肠毒素B的一种更大的膜结合形式是细胞外肠毒素B的动力学前体。肠毒素B前体分子的加工显然可以在共翻译或翻译后发生。细胞的亚细胞分级分离显示,所有前体毒素都与膜部分相关。一旦从前体加工并从膜中释放出来,它在释放到细胞外环境之前会短暂地与细胞壁结合。细胞壁结合的肠毒素B对蛋白酶处理以及在0至2摄氏度下用高盐或低盐溶液提取完全具有抗性,尽管通过用溶葡萄球菌素去除细胞壁可以很容易地将其从细胞中释放出来。这些数据表明,新形成的肠毒素B在释放到细胞外环境之前可能会暂时隔离在需要细胞壁完整性的特殊区域中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/845a/217370/041cee4901d7/jbacter00248-0321-a.jpg

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