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首页> 外文期刊>Scientific reports. >Cosmid based mutagenesis causes genetic instability in Streptomyces coelicolor, as shown by targeting of the lipoprotein signal peptidase gene
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Cosmid based mutagenesis causes genetic instability in Streptomyces coelicolor, as shown by targeting of the lipoprotein signal peptidase gene

机译:如通过靶向脂蛋白信号肽酶基因所示,基于粘粒的诱变会导致天蓝色链霉菌的遗传不稳定

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Bacterial lipoproteins are extracellular proteins tethered to cell membranes by covalently attached lipids. Deleting the lipoprotein signal peptidase (lsp) gene in Streptomyces coelicolor results in growth and developmental defects that cannot be restored by reintroducing lsp. This led us to hypothesise that lsp is essential and that the lsp mutant we isolated previously had acquired compensatory secondary mutations. Here we report resequencing of the genomes of wild-type M145 and the cis-complemented ?lsp mutant (BJT1004) to map and identify these secondary mutations but we show that they do not increase the efficiency of disrupting lsp and are not lsp suppressors. We provide evidence that they are induced by introducing the cosmid St4A10?lsp, as part of ReDirect PCR mutagenesis protocol, which transiently duplicates a number of important cell division genes. Disruption of lsp using a suicide vector (which does not result in gene duplication) still results in growth and developmental delays and we conclude that loss of Lsp function results in developmental defects due to the loss of all lipoproteins from the cell membrane. Significantly, our results also indicate the use of cosmid libraries for the genetic manipulation of bacteria can lead to phenotypes not necessarily linked to the gene(s) of interest.
机译:细菌脂蛋白是通过共价附着的脂质与细胞膜束缚的细胞外蛋白。删除天蓝色链霉菌中的脂蛋白信号肽酶(lsp)基因会导致生长和发育缺陷,而不能通过重新引入lsp来恢复。这导致我们假设lsp是必不可少的,而我们先前分离出的lsp突变体已经获得了补偿性二级突变。在这里,我们报告了野生型M145和顺式互补的llsp突变体(BJT1004)的基因组重测序,以定位和鉴定这些次级突变,但我们表明它们不会增加破坏lsp的效率,并且不是lsp抑制子。我们提供的证据表明,它们是通过引入粘粒St4A10?lsp(作为ReDirect PCR诱变协议的一部分)而诱导的,该协议可瞬时复制许多重要的细胞分裂基因。使用自杀载体破坏lsp(不会导致基因重复)仍然会导致生长和发育延迟,并且我们得出结论,由于细胞膜上所有脂蛋白的损失,Lsp功能的丧失会导致发育缺陷。重要的是,我们的结果还表明,将粘粒文库用于细菌的遗传操作可能会导致表型不一定与目标基因相关。

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