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Development of a Tunable Wide-Range Gene Induction System Useful for the Study of Streptococcal Toxin-Antitoxin Systems

机译:可调节的广谱基因诱导系统的开发,可用于研究链球菌毒素-抗毒素系统

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Despite the plethora of genetic tools that have been developed for use in Streptococcus mutans , the S. mutans genetic system still lacks an effective gene induction system exhibiting low basal expression and strong inducibility. Consequently, we created two hybrid gene induction cassettes referred to as Xyl-S1 and Xyl-S2. Both Xyl-S cassettes are xylose inducible and controlled by the Bacillus megaterium xylose repressor. The Xyl-S cassettes each demonstrated >600-fold-increased reporter activity in the presence of 1.2% (wt/vol) xylose. However, the Xyl-S1 cassette yielded a much higher maximum level of gene expression, whereas the Xyl-S2 cassette exhibited much lower uninduced basal expression. The cassettes also performed similarly in Streptococcus sanguinis and Streptococcus gordonii , which suggests that they are likely to be useful in a variety of streptococci. We demonstrate how both Xyl-S cassettes are particularly useful for the study of toxin-antitoxin (TA) modules using both the previously characterized S. mutans mazEF TA module and a previously uncharacterized HicAB TA module in S. mutans . HicAB TA modules are widely distributed among bacteria and archaea, but little is known about their function. We show that HicA serves as the toxin component of the module, while HicB serves as the antitoxin. Our results suggest that, in contrast to that of typical TA modules, HicA toxicity in S. mutans is modest at best. The implications of these results for HicAB function are discussed.
机译:尽管已经开发出许多用于变形链球菌的遗传工具,但是变形链球菌的遗传系统仍缺乏有效的基因诱导系统,该系统具有低基础表达和强诱导性。因此,我们创建了两个杂种基因诱导盒,分别称为Xyl-S1和Xyl-S2。两个Xyl-S盒都是木糖诱导型的,并由巨大芽孢杆菌木糖阻遏物控制。在1.2%(wt / vol)木糖的存在下,每个Xyl-S盒均显示出> 600倍的报告基因活性。但是,Xyl-S1盒产生更高的最大基因表达水平,而Xyl-S2盒表现出更低的未诱导基础表达。盒式磁带在血链球菌和戈登链球菌中的表现也相似,这表明它们可能在多种链球菌中有用。我们展示了两个Xyl-S盒如何特别适用于使用变形链球菌的先前表征的变形链球菌mazEF TA模块和先前未表征的HicAB TA模块的毒素-抗毒素(TA)模块的研究。 HicAB TA模块广泛分布于细菌和古细菌中,但对其功能知之甚少。我们显示,HicA充当模块的毒素成分,而HicB充当抗毒素。我们的结果表明,与典型的TA模块相比,变形链球菌的HicA毒性充其量仅是适度的。讨论了这些结果对HicAB功能的影响。

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