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大肠杆菌STA3热稳定肠毒素的分泌:Pro-STA的细胞外递送可通过Pro或STA完成。

Secretion of the STA3 heat-stable enterotoxin of Escherichia coli: extracellular delivery of Pro-STA is accomplished by either Pro or STA.

作者信息

Yang Y, Gao Z, Guzmán-Verduzco L M, Tachias K, Kupersztoch Y M

机构信息

Department of Microbiology, University of Texas Southwestern Medical Center, Dallas 75235-9048.

出版信息

Mol Microbiol. 1992 Dec;6(23):3521-9. doi: 10.1111/j.1365-2958.1992.tb01787.x.

DOI:10.1111/j.1365-2958.1992.tb01787.x
PMID:1474896
Abstract

The methanol-soluble, heat-stable enterotoxin of Escherichia coli is a protease-resistant extracellular peptide which is synthesized as a 72-amino-acid precursor Pre-Pro-STA3. The specific roles of Pre (19 amino acids), Pro (34 amino acids) and STA3 (19 amino acids) in the secretion process were studied by functionally deleting each of the three domains. Deletion of the Pre signal sequence resulted in a short-lived cell-associated molecule with an M(r) equivalent to that of Pro-STA3. Deletion of Pro (i.e., Pre-STA3) resulted in the rapid extracellular accumulation of STA3; the periplasmic intermediate found in the secretion of the wild-type toxin was undetected. Deletion of the STA3 domain resulted in a cell-associated Pre-Pro peptide; with time this form converted to periplasmic Pro which later became extracellular. When DNA encoding either STA3, by itself, or Pro-STA3 (lacking the signal peptide) was expressed, these peptides were degraded intracellularly, with no periplasmic or extracellular forms detected. The results presented demonstrate that the signal peptide (Pre) is essential even for the export of small peptides to the periplasm, and that its absence causes the STA3 domain to become susceptible to intracellular proteases. The rapid degradation of intracellular STA3 indicates that its proteolytic resistance is acquired in a compartment other than the cytoplasm. The results also show that after the Pre domain is proteolytically cleaved from Pre-STA3 and Pre-Pro, the STA3 and Pro peptides can exit to the culture supernatant.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

大肠杆菌的甲醇可溶、热稳定肠毒素是一种抗蛋白酶的细胞外肽,它作为一种72个氨基酸的前体Pre-Pro-STA3合成。通过功能缺失三个结构域中的每一个,研究了Pre(19个氨基酸)、Pro(34个氨基酸)和STA3(19个氨基酸)在分泌过程中的具体作用。缺失Pre信号序列导致产生一种寿命短暂的细胞相关分子,其分子量与Pro-STA3相当。缺失Pro(即Pre-STA3)导致STA3在细胞外快速积累;未检测到野生型毒素分泌过程中发现的周质中间体。缺失STA3结构域导致产生一种细胞相关的Pre-Pro肽;随着时间的推移,这种形式转变为周质Pro,随后变为细胞外形式。当单独表达编码STA3或Pro-STA3(缺乏信号肽)的DNA时,这些肽在细胞内被降解,未检测到周质或细胞外形式。所呈现的结果表明,信号肽(Pre)即使对于小肽输出到周质也是必不可少的,并且其缺失会导致STA3结构域易受细胞内蛋白酶的作用。细胞内STA3的快速降解表明其抗蛋白酶能力是在细胞质以外的区室中获得的。结果还表明,在Pre结构域从Pre-STA3和Pre-Pro上被蛋白酶切割后,STA3和Pro肽可以分泌到培养上清液中。(摘要截短至250字)

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