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镓(III)-水杨醛缩邻氨基酚作为血红素感知和铁摄取的双重抑制剂

Gallium(III)-Salophen as a Dual Inhibitor of Heme Sensing and Iron Acquisition.

作者信息

Centola Garrick, Deredge Daniel J, Hom Kellie, Ai Yong, Dent Alecia T, Xue Fengtian, Wilks Angela

机构信息

Department of Pharmaceutical Sciences, University of Maryland School of Pharmacy, Baltimore, Maryland 21201, United States.

出版信息

ACS Infect Dis. 2020 Aug 14;6(8):2073-2085. doi: 10.1021/acsinfecdis.0c00138. Epub 2020 Jul 6.

Abstract

is an opportunistic bacterium that causes life-threatening infections in immunocompromised patients. In infection, it uses heme as a primary iron source and senses the availability of exogenous heme through the heme assimilation system (Has), an extra cytoplasmic function σ-factor system. A secreted hemophore HasAp scavenges heme and, upon interaction with the outer-membrane receptor HasR, activates a signaling cascade, which in turn creates a positive feedback loop critical for sensing and adaptation within the host. The ability to sense and respond to heme as an iron source contributes to virulence. Consequently, the inhibition of this system will lead to a disruption in iron homeostasis, decreasing virulence. We have identified a salophen scaffold that successfully inhibits the activation of the Has signaling system while simultaneously targeting iron uptake via xenosiderophore receptors. We propose this dual mechanism wherein free Ga-salophen reduces growth through uptake and iron mimicry. A dual mechanism targeting extracellular heme signaling and uptake together with Ga-induced toxicity following active Gasalophen uptake provides a significant therapeutic advantage while reducing the propensity to develop resistance.

摘要

是一种机会致病菌,可在免疫功能低下的患者中引起危及生命的感染。在感染过程中,它利用血红素作为主要铁源,并通过血红素同化系统(Has)感知外源性血红素的可用性,该系统是一种胞外功能σ因子系统。分泌的血红蛋白载体HasAp清除血红素,并在与外膜受体HasR相互作用时激活信号级联反应,进而产生一个正反馈回路,这对于在宿主体内的感知和适应至关重要。将血红素作为铁源进行感知和响应的能力有助于其毒力。因此,抑制该系统将导致铁稳态的破坏,降低毒力。我们已经鉴定出一种沙罗芬支架,它成功地抑制了Has信号系统的激活,同时通过异源铁载体受体靶向铁摄取。我们提出这种双重机制,即游离的镓-沙罗芬通过摄取和铁模拟来减少生长。针对细胞外血红素信号传导和摄取的双重机制,以及活性镓-沙罗芬摄取后镓诱导的毒性,提供了显著的治疗优势,同时降低了产生耐药性的倾向。

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