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革兰氏阴性菌蛋白质分泌机制:铜绿假单胞菌外毒素A

Mechanism of protein excretion by gram-negative bacteria: Pseudomonas aeruginosa exotoxin A.

作者信息

Lory S, Tai P C, Davis B D

出版信息

J Bacteriol. 1983 Nov;156(2):695-702. doi: 10.1128/jb.156.2.695-702.1983.

Abstract

Excretion of proteins by a cell with a double membrane may involve mechanisms different from secretion across a single membrane. We studied this problem with Pseudomonas aeruginosa exotoxin A. This 68,000-dalton protein was released as rapidly as it was completed; even after short pulse-labeling the cells contained neither the toxin nor a larger precursor. Excretion is evidently cotranslational, since in fractionated lysates the toxin was formed (almost entirely in the mature form) by the membrane-polysome complexes but not by the free polysomes. When the membrane was perturbed by 10% ethanol, the cells stopped excreting the toxin and they accumulated an immunoprecipitable, enzymatically active precursor of 71,000 daltons. The precursor was located entirely in the outer membrane on its outer surface. On removal of the ethanol, the cells again excreted mature toxin, but they did not process or release the previously accumulated precursor. Based on these data, a model for the excretion of exotoxin A is presented.

摘要

具有双层膜的细胞排出蛋白质的机制可能不同于通过单层膜的分泌机制。我们用铜绿假单胞菌外毒素A研究了这个问题。这种68,000道尔顿的蛋白质一完成就迅速释放;即使经过短时间脉冲标记,细胞中既没有毒素也没有更大的前体。排泄显然是共翻译的,因为在分级分离的裂解物中,毒素是由膜 - 多核糖体复合物形成的(几乎完全是成熟形式),而不是由游离多核糖体形成的。当膜被10%乙醇扰动时,细胞停止排出毒素,并积累了一种71,000道尔顿的可免疫沉淀、具有酶活性的前体。前体完全位于外膜的外表面。去除乙醇后,细胞再次排出成熟毒素,但它们没有加工或释放先前积累的前体。基于这些数据,提出了外毒素A的排泄模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1fe/217885/4584e3fb5a55/jbacter00240-0228-a.jpg

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