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Ru(CO)3Cl(Glycinate) (CORM-3): A Carbon Monoxide–Releasing Molecule with Broad-Spectrum Antimicrobial and Photosensitive Activities Against Respiration and Cation Transport in Escherichia coli

机译:Ru(CO)3Cl(甘氨酸)(CORM-3):一氧化碳释放分子具有广谱抗菌和光敏活性可抵抗大肠杆菌中的呼吸和阳离子转运。

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摘要

>Aims: Carbon monoxide (CO) delivered to cells and tissues by CO-releasing molecules (CO-RMs) has beneficial and toxic effects not mimicked by CO gas. The metal carbonyl Ru(CO)3Cl(glycinate) (CORM-3) is a novel, potent antimicrobial agent. Here, we established its mode of action. >Results: CORM-3 inhibits respiration in several bacterial and yeast pathogens. In anoxic Escherichia coli suspensions, CORM-3 first stimulates, then inhibits respiration, but much higher concentrations of CORM-3 than of a classic protonophore are required for stimulation. Proton translocation measurements (H+/O quotients, i.e., H+ extrusion on pulsing anaerobic cells with O2) show that respiratory stimulation cannot be attributed to true “uncoupling,” that is, dissipation of the protonmotive force, or to direct stimulation of oxidase activity. Our data are consistent with CORM-3 facilitating the electrogenic transmembrane movement of K+ (or Na+), causing a stimulation of respiration and H+ pumping to compensate for the transient drop in membrane potential (ΔΨ). The effects on respiration are not mimicked by CO gas or control Ru compounds that do not release CO. Inhibition of respiration and loss of bacterial viability elicited by CORM-3 are reversible by white light, unambiguously identifying heme-containing oxidase(s) as target(s). >Innovation: This is the most complete study to date of the antimicrobial action of a CO-RM. Noteworthy are the demonstration of respiratory stimulation, electrogenic ion transport, and photosensitive activity, establishing terminal oxidases and ion transport as primary targets. >Conclusion: CORM-3 has multifaceted effects: increased membrane permeability, inhibition of terminal oxidases, and perhaps other unidentified mechanisms underlie its effectiveness in tackling microbial pathogenesis. Antioxid. Redox Signal. 19, 497–509.
机译:>目标:通过释放CO的分子(CO-RM)传递到细胞和组织中的一氧化碳(CO)具有有益和有毒的作用,不能被CO气体模仿。羰基金属Ru(CO)3Cl(甘氨酸盐)(CORM-3)是一种新型的有效抗菌剂。在这里,我们建立了它的行动方式。 >结果:CORM-3抑制几种细菌和酵母病原体的呼吸。在缺氧的大肠杆菌悬浮液中,CORM-3首先刺激,然后抑制呼吸,但是刺激所需的浓度比经典质子体高得多。质子易位测量(H + / O商,即在带有O2的脉冲厌氧细胞上的H + 挤压)表明,呼吸刺激不能归因于真正的“解偶联”,即即,质子动力的耗散或直接刺激氧化酶活性。我们的数据与CORM-3促进K + (或Na + )的电跨膜运动,从而刺激呼吸和H + 抽水以补偿膜电位(ΔΨ)的瞬时下降。对呼吸的影响不会被一氧化碳气体或不释放一氧化碳的对照钌化合物所模仿。白光可以逆转由CORM-3引起的呼吸抑制和细菌生存力丧失,明确确定含血红素的氧化酶为目标(s)。 >创新:这是迄今为止关于CO-RM抗菌作用的最完整的研究。值得注意的是对呼吸刺激,电离子迁移和光敏活性的演示,建立了末端氧化酶和离子迁移作为主要目标。 >结论:CORM-3具有多方面的作用:增加膜的通透性,抑制末端氧化酶,以及其他未知机制,可能是其解决微生物发病机理的基础。抗氧化。氧化还原信号。 19,497–509。

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