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细菌中的金属稳态:ArsR-SmtB转录阻遏物家族在应对环境中不同金属浓度时的作用

Metal homeostasis in bacteria: the role of ArsR-SmtB family of transcriptional repressors in combating varying metal concentrations in the environment.

作者信息

Saha Rudra P, Samanta Saikat, Patra Surajit, Sarkar Diganta, Saha Abinit, Singh Manoj Kumar

机构信息

Department of Biotechnology, School of Biotechnology, Adamas University, Kolkata, 700126, India.

Department of Microbiology, School of Science, Adamas University, Kolkata, 700126, India.

出版信息

Biometals. 2017 Aug;30(4):459-503. doi: 10.1007/s10534-017-0020-3. Epub 2017 May 16.

DOI:10.1007/s10534-017-0020-3
PMID:28512703
Abstract

Bacterial infections cause severe medical problems worldwide, resulting in considerable death and loss of capital. With the ever-increasing rise of antibiotic-resistant bacteria and the lack of development of new antibiotics, research on metal-based antimicrobial therapy has now gained pace. Metal ions are essential for survival, but can be highly toxic to organisms if their concentrations are not strictly controlled. Through evolution, bacteria have acquired complex metal-management systems that allow them to acquire metals that they need for survival in different challenging environments while evading metal toxicity. Metalloproteins that controls these elaborate systems in the cell, and linked to key virulence factors, are promising targets for the anti-bacterial drug development. Among several metal-sensory transcriptional regulators, the ArsR-SmtB family displays greatest diversity with several distinct metal-binding and nonmetal-binding motifs that have been characterized. These prokaryotic metolloregulatory transcriptional repressors represses the expression of operons linked to stress-inducing concentrations of metal ions by directly binding to the regulatory regions of DNA, while derepression results from direct binding of metal ions by these homodimeric proteins. Many bacteria, e.g., Mycobacterium tuberculosis, Bacillus anthracis, etc., have evolved to acquire multiple metal-sensory motifs which clearly demonstrate the importance of regulating concentrations of multiple metal ions. Here, we discussed the mechanisms of how ArsR-SmtB family regulates the intracellular bioavailability of metal ions both inside and outside of the host. Knowledge of the metal-challenges faced by bacterial pathogens and their survival strategies will enable us to develop the next generation drugs.

摘要

细菌感染在全球范围内引发严重的医学问题,导致大量死亡和资金损失。随着抗生素耐药菌的不断增加以及新抗生素研发的匮乏,基于金属的抗菌疗法研究如今已加速推进。金属离子对生物生存至关重要,但如果其浓度不受严格控制,可能对生物体具有高毒性。通过进化,细菌获得了复杂的金属管理系统,使它们能够在不同具有挑战性的环境中获取生存所需的金属,同时规避金属毒性。在细胞中控制这些精细系统并与关键毒力因子相关联的金属蛋白,是抗菌药物开发的有前景的靶点。在几种金属感应转录调节因子中,ArsR-SmtB家族表现出最大的多样性,具有几个已被表征的不同金属结合和非金属结合基序。这些原核金属调节转录抑制因子通过直接结合DNA的调控区域来抑制与应激诱导浓度的金属离子相关的操纵子的表达,而这些同二聚体蛋白与金属离子的直接结合则导致去抑制。许多细菌,如结核分枝杆菌、炭疽芽孢杆菌等,已经进化出获得多个金属感应基序,这清楚地证明了调节多种金属离子浓度的重要性。在这里,我们讨论了ArsR-SmtB家族如何调节宿主内外金属离子的细胞内生物利用度的机制。了解细菌病原体面临的金属挑战及其生存策略将使我们能够开发下一代药物。

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