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Signal peptide etiquette during assembly of a complex respiratory enzyme

机译:复杂呼吸酶组装过程中的信号肽礼节

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摘要

Summary: Salmonella enterica serovar Typhimurium is a Gram-negative pathogen capable of respiration with a number of terminal electron acceptors. Tetrathionate reductase is important for the infection process and is encoded by the ttrBCA operon where TtrA and TtrB are metallocofactor-containing proteins targeted to the periplasmic side of the membrane by two different Tat targeting peptides. In this work, the inter-relationship between these two signal peptides has been explored. Molecular genetics and biochemical approaches reveal that the processing of the TtrB Tat signal peptide is dependent on the successful assembly of its partner protein, TtrA. Inactivation of either the TtrA or the TtrB Tat targeting peptides individually was observed to have limited overall effects on assembly of the enzyme or on cellular tetrathionate reductase activity. However, inactivation of both signal peptides simultaneously was found to completely abolish physiological tetrathionate reductase activity. These data suggest both signals are normally active during assembly of the enzyme, and imply a code of conduct exists between the signal peptides where one can compensate for inactivity in the other. Since it appears likely that tetrathionate reductase presents itself for export as a multi-signal complex, these observations also have implications for the mechanism of the bacterial Tat translocase.
机译:摘要:肠炎沙门氏菌鼠伤寒沙门氏菌是革兰氏阴性病原体,能够通过许多末端电子受体进行呼吸。四硫酸盐还原酶对感染过程很重要,由ttrBCA操纵子编码,其中TtrA和TtrB是含金属因子的蛋白质,被两种不同的Tat靶向肽靶向到膜的周质侧。在这项工作中,已经探索了这两个信号肽之间的相互关系。分子遗传学和生物化学方法表明,TtrB Tat信号肽的加工取决于其伴侣蛋白TtrA的成功组装。观察到分别灭活TtrA或TtrB Tat靶向肽对酶的组装或细胞四硫酸盐还原酶活性的总体作用有限。然而,发现两个信号肽的同时失活完全消除了生理学四硫酸盐还原酶活性。这些数据表明,两种信号在酶的组装过程中通常都是有活性的,并且暗示在信号肽之间存在行为准则,其中一种信号肽可以补偿另一种信号的失活。由于四硫酸盐还原酶似乎很可能以多信号复合物形式输出,因此这些观察结果也对细菌Tat转位酶的机制有影响。

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