Park Jong, Ryu So-Yeon, Kim Choon-Mee, Shin Sung-Heui
Research Center for Resistant Cells, Chosun University Medical School, Gwangju, Republic of Korea.
J Microbiol. 2008 Jun;46(3):338-43. doi: 10.1007/s12275-008-0058-6. Epub 2008 Jul 5.
Vibrio vulnificus has been known to secrete one form of metalloprotease VvpE (45 kDa) that is cleaved to 34 kDa-VvpE and 11 kDa-C-terminal propeptide via extracellular autoproteolysis. However, we found that extracellular secretion of both the 34 and 45 kDa forms of VvpE began in the early growth phase; moreover, 34 kDa-VvpE existed as the major form in V. vulnificus cell lysates and culture supernatants. In addition, extracellular secretion of both 34 and 45 kDa-VvpE was blocked by mutation of the pilD gene, which encodes for the type IV leader peptidase/N-methyltransferase of the type II general secretion system, and the blocked VvpE secretion was recovered by in trans-complementation of the wild-type pilD gene. These results indicate that 34 kDa-VvpE is the major form secreted along with 45 kDa-VvpE from the early growth phase via the PilD-mediated type II general secretion system.
已知创伤弧菌会分泌一种金属蛋白酶VvpE(45 kDa),该酶通过细胞外自蛋白水解作用裂解为34 kDa-VvpE和11 kDa-C末端前肽。然而,我们发现34 kDa和45 kDa形式的VvpE在生长早期就开始进行细胞外分泌;此外,34 kDa-VvpE是创伤弧菌细胞裂解物和培养上清液中的主要形式。另外,pilD基因发生突变会阻断34 kDa和45 kDa-VvpE的细胞外分泌,该基因编码II型通用分泌系统的IV型前导肽酶/N-甲基转移酶,而通过野生型pilD基因的反式互补可恢复被阻断的VvpE分泌。这些结果表明,34 kDa-VvpE是从生长早期开始通过PilD介导的II型通用分泌系统与45 kDa-VvpE一起分泌的主要形式。
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