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首页> 外文期刊>Journal of bacteriology >In vitro interactions of CysB protein with the cysJIH promoter of Salmonella typhimurium: inhibitory effects of sulfide.
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In vitro interactions of CysB protein with the cysJIH promoter of Salmonella typhimurium: inhibitory effects of sulfide.

机译:CysB蛋白与鼠伤寒沙门氏菌cysJIH启动子的体外相互作用:硫化物的抑制作用。

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The cysteine regulon of Salmonella typhimurium is positively regulated by the CysB protein and an inducer, which can be either O-acetyl-L-serine or N-acetyl-L-serine. In vivo experiments confirmed that sulfide and L-cysteine (supplied as L-cystine) interfere with induction by exogenously supplied O-acetyl-L-serine and also showed the same effects when N-acetyl-L-serine was used as an inducer. In a gel shift assay, purified CysB protein bound specifically to a 278-base-pair DNA fragment containing the S. typhimurium cysJIH promoter region. Binding occurred in the absence of inducer but did not stimulate in vitro transcription initiation, indicating that binding alone is insufficient to cause formation of a transcription initiation complex. Addition of N-acetyl-L-serine or O-acetyl-L-serine was required for transcription initiation and also stimulated binding three- to eightfold. Sulfide inhibited both transcription initiation and binding by interfering with the stimulatory effects of inducer in a competitive manner. These findings indicate that sulfide is an anti-inducer and may explain why full expression of the cysteine regulon requires sulfur limitation. L-Cysteine did not affect in vitro transcription initiation or binding of CysB protein to the cysJIH promoter region. The in vivo effects of L-cysteine may be secondary to its degradation to sulfide by the inducible enzyme cysteine desulfhydrase.
机译:鼠伤寒沙门氏菌的半胱氨酸调节因子由CysB蛋白和诱导剂正调控,诱导剂可以是O-乙酰基-L-丝氨酸或N-乙酰基-L-丝氨酸。体内实验证实,硫化物和L-半胱氨酸(作为L-胱氨酸提供)会干扰外源供应的O-乙酰基-L-丝氨酸的诱导作用,当使用N-乙酰基-L-丝氨酸作为诱导剂时,也显示出相同的作用。在凝胶迁移分析中,纯化的CysB蛋白与含有鼠伤寒沙门氏菌cysJIH启动子区域的278个碱基对的DNA片段特异性结合。在不存在诱导剂的情况下发生结合,但不刺激体外转录起始,这表明单独的结合不足以引起转录起始复合物的形成。转录起始需要添加N-乙酰基-L-丝氨酸或O-乙酰基-L-丝氨酸,并且还刺激三至八倍的结合。硫化物通过竞争性干扰诱导物的刺激作用抑制转录起始和结合。这些发现表明硫化物是抗诱导剂,并且可以解释为什么半胱氨酸调节子的完整表达需要硫限制。 L-半胱氨酸不影响体外转录起始或CysB蛋白与cysJIH启动子区域的结合。 L-半胱氨酸的体内作用可能是继可诱导酶半胱氨酸脱硫酶降解为硫化物之后的继发作用。

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