首页> 外文OA文献 >New Insights into the Cyclic di-Adenosine Monophosphate (c-di-AMP) Degradation Pathway and the Requirement of the Cyclic-Dinucleotide for Acid Stress Resistance in Staphylococcus aureus.
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New Insights into the Cyclic di-Adenosine Monophosphate (c-di-AMP) Degradation Pathway and the Requirement of the Cyclic-Dinucleotide for Acid Stress Resistance in Staphylococcus aureus.

机译:对环金属二磷酸腺苷(c-di-amp)降解途径的新见解及环状二核苷酸对金黄色葡萄球菌耐酸性的要求。

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摘要

Nucleotide signaling networks are key to facilitate alterations in gene expression, protein function and enzyme activity in response to diverse stimuli. Cyclic di-adenosine monophosphate (c-di-AMP) is an important secondary messenger molecule produced by the human pathogen Staphylococcus aureus and is involved in regulating a number of physiological processes including potassium transport. S. aureus must ensure tight control over its cellular levels as both high levels of the dinucleotide and its absence result in a number of detrimental phenotypes. Here we show that in addition to the membrane bound Asp-His-His and Asp-His-His associated (DHH/DHHA1) domain-containing phosphodiesterase (PDE) GdpP, S. aureus produces a second cytoplasmic DHH/DHHA1 PDE Pde2. Although capable of hydrolyzing c-di-AMP, Pde2 preferentially converts linear 5-phosphadenylyl-adenosine (pApA) to AMP. Using a pde2 mutant strain, pApA was detected for the first time in S. aureus, leading us to speculate that this dinucleotide may have a regulatory role under certain conditions. Moreover, pApA is involved in a feedback inhibition loop that limits GdpP-dependent c-di-AMP hydrolysis. Another protein linked to the regulation of c-di-AMP levels in bacteria is the predicted regulator protein YbbR. Here, it is shown that a ybbR mutant S. aureus strain has increased acid sensitivity that can be bypassed by the acquisition of mutations in a number of genes, including the gene coding for the diadenylate cyclase DacA. We further show that c-di-AMP levels are slightly elevated in the ybbR suppressor strains tested as compared to the wild-type strain. With this, we not only identified a new role for YbbR in acid stress resistance in S. aureus, but also provide further insight into how c-di-AMP levels impact acid tolerance in this organism.
机译:核苷酸信号转导网络是促进基因表达,蛋白质功能和酶活性响应各种刺激变化的关键。环状单磷酸二腺苷(c-di-AMP)是人类病原体金黄色葡萄球菌产生的重要二级信使分子,参与调节包括钾转运在内的许多生理过程。金黄色葡萄球菌必须确保对其细胞水平的严格控制,因为高水平的二核苷酸及其缺乏都会导致许多有害的表型。在这里我们显示,除了与膜结合的Asp-His-His和与Asp-His-His相关的(DHH / DHHA1)域含磷酸二酯酶(PDE)GdpP,金黄色葡萄球菌还产生第二个细胞质DHH / DHHA1 PDE Pde2。尽管能够水解c-di-AMP,但Pde2优先将线性5-磷腺苷基腺苷(pApA)转化为AMP。使用pde2突变株,在金黄色葡萄球菌中首次检测到pApA,这使我们推测该二核苷酸在某些条件下可能具有调节作用。此外,pApA参与了一个反馈抑制回路,该回路限制了GdpP依赖的c-di-AMP水解。与细菌中c-di-AMP水平的调节有关的另一种蛋白是预测的调节蛋白YbbR。在这里,显示出ybbR突变体金黄色葡萄球菌菌株具有增加的酸敏感性,其可以通过许多基因的突变而被绕开,包括编码二腺苷酸环化酶DacA的基因。我们进一步显示,与野生型菌株相比,在测试的ybbR抑制菌株中c-di-AMP的含量略有提高。这样,我们不仅确定了YbbR在金黄色葡萄球菌的耐酸胁迫中的新作用,而且还提供了有关c-di-AMP水平如何影响该生物体耐酸性的进一步见解。

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