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一氧化碳释放分子-3(CORM-3;Ru(CO)3Cl(甘氨酸盐))作为研究一氧化碳和一氧化氮对细菌黄素血红蛋白Hmp协同作用的工具:应用与陷阱

Carbon monoxide-releasing molecule-3 (CORM-3; Ru(CO)3Cl(glycinate)) as a tool to study the concerted effects of carbon monoxide and nitric oxide on bacterial flavohemoglobin Hmp: applications and pitfalls.

作者信息

Tinajero-Trejo Mariana, Denby Katie J, Sedelnikova Svetlana E, Hassoubah Shahira A, Mann Brian E, Poole Robert K

机构信息

From the Departments of Molecular Biology & Biotechnology and

From the Departments of Molecular Biology & Biotechnology and.

出版信息

J Biol Chem. 2014 Oct 24;289(43):29471-82. doi: 10.1074/jbc.M114.573444. Epub 2014 Sep 5.

Abstract

CO and NO are small toxic gaseous molecules that play pivotal roles in biology as gasotransmitters. During bacterial infection, NO, produced by the host via the inducible NO synthase, exerts critical antibacterial effects while CO, generated by heme oxygenases, enhances phagocytosis of macrophages. In Escherichia coli, other bacteria and fungi, the flavohemoglobin Hmp is the most important detoxification mechanism converting NO and O2 to the ion nitrate (NO3(-)). The protoheme of Hmp binds not only O2 and NO, but also CO so that this ligand is expected to be an inhibitor of NO detoxification in vivo and in vitro. CORM-3 (Ru(CO)(3)Cl(glycinate)) is a metal carbonyl compound extensively used and recently shown to have potent antibacterial properties. In this study, attenuation of the NO resistance of E. coli by CORM-3 is demonstrated in vivo. However, polarographic measurements showed that CO gas, but not CORM-3, produced inhibition of the NO detoxification activity of Hmp in vitro. Nevertheless, CO release from CORM-3 in the presence of soluble cellular compounds is demonstrated by formation of carboxy-Hmp. We show that the inability of CORM-3 to inhibit the activity of purified Hmp is due to slow release of CO in protein solutions alone i.e. when sodium dithionite, widely used in previous studies of CO release from CORM-3, is excluded. Finally, we measure intracellular CO released from CORM-3 by following the formation of carboxy-Hmp in respiring cells. CORM-3 is a tool to explore the concerted effects of CO and NO in vivo.

摘要

一氧化碳(CO)和一氧化氮(NO)是具有毒性的小分子气体,作为气体信号分子在生物学中发挥着关键作用。在细菌感染期间,宿主通过诱导型一氧化氮合酶产生的NO发挥关键的抗菌作用,而血红素加氧酶产生的CO则增强巨噬细胞的吞噬作用。在大肠杆菌、其他细菌和真菌中,黄素血红蛋白Hmp是将NO和O2转化为硝酸根离子(NO3(-))的最重要解毒机制。Hmp的原血红素不仅能结合O2和NO,还能结合CO,因此这种配体有望在体内和体外抑制NO解毒。三羰基氯化钌(甘氨酸)(CORM-3)是一种广泛使用的金属羰基化合物,最近被证明具有强大的抗菌性能。在本研究中,体内实验证明CORM-3可减弱大肠杆菌对NO的抗性。然而,极谱测量表明,在体外,是CO气体而非CORM-3抑制了Hmp的NO解毒活性。尽管如此,通过羧基-Hmp的形成证明了在可溶性细胞化合物存在下CORM-3会释放CO。我们表明,CORM-3无法抑制纯化的Hmp的活性是由于仅在蛋白质溶液中CO释放缓慢,即在排除先前CORM-3释放CO研究中广泛使用的连二亚硫酸钠的情况下。最后,我们通过追踪呼吸细胞中羧基-Hmp的形成来测量CORM-3释放的细胞内CO。CORM-3是一种在体内探索CO和NO协同作用的工具。

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