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受自然界在氧化环境中获取铁的启发而设计和合成新型抗生素。

Design and Syntheses of New Antibiotics Inspired by Nature's Quest for Iron in an Oxidative Climate.

机构信息

Department of Chemistry and Biochemistry, University of Notre Dame, Notre Dame, Indiana 46556, United States.

出版信息

Acc Chem Res. 2021 Apr 6;54(7):1646-1661. doi: 10.1021/acs.accounts.1c00004. Epub 2021 Mar 8.

Abstract

This Account describes fundamental chemistry that promoted the discovery of new antibiotics. Specifically, the NH acidity of simple hydroxamic acid derivatives facilitated the syntheses of novel β-lactams (oxamazins and monobactams), siderophore mimics that limit bacterial iron uptake and bacterially targeted sideromycins (siderophore-antibiotic conjugates). The development of resistance to our current limited set of antibiotic scaffolds has created a dire medical situation. As recently stated, "if you weren't taking antibiotic resistance seriously before, now would be a good time to start." A project commissioned by the British government (https://amr-review.org/) has released estimates of the near-future global toll of antibiotic resistance that are jaw-dropping in their seriousness and scale: 10 million deaths per year and at least $100 trillion in sacrificed gross national product. The 2020 COVID pandemic confirmed that infectious disease problems are no longer localized but worldwide. Many classical antibiotics, especially β-lactams, previously provided economical cures, but the evolution of antibiotic destructive enzymes (i.e., β-lactamases), efflux pumps, and bacterial cell wall permeability barriers has made many types of bacteria, especially Gram-negative strains, resistant. Still, and in contrast to other therapies, the public expectation is that any new antibiotic must be inexpensive. This creates market limitations that have caused most major pharmaceutical companies to abandon antibiotic research. Much needs to be done to address this significant problem.The critical need for bacteria to sequester essential iron provides an Achilles' heel for new antibiotic development. Although ferric iron is extremely insoluble, bacteria need micromolar intracellular concentrations for growth and virulence. To this end, they biosynthesize siderophores (Gr. iron bearer) and excrete them into their environment, where they bind iron with high affinity. The iron complexes are recognized by specific outer-membrane transporters, and once actively internalized, the iron is released for essential processes. To conserve biosynthetic energy, some bacteria recognize and utilize siderophores made by competing strains. As a counter-revolution in the never-ending fight for survival, bacteria have also evolved sideromycins, which are siderophores conjugated to warheads that are lethal to rogue bacteria. While none are now used therapeutically, natural sideromycins called albomycins have been used clinically, and others have been shown to be well tolerated and active in animal infection models. Herein we describe practical methods to synthesize new antibiotics and artificial sideromycins with the generalized structure shown above (siderophore-linker drug). Utilizing the molecular-recognition-based siderophore/sideromycin bacterial assimilation processes, it is possible to design both broad spectrum and exquisitely narrow spectrum (targeted) sideromycins and even repurpose older or more classical antibiotics. Relevant microbiological assays, animal infection studies, and the recent FDA approval of cefiderocol demonstrate their effectiveness.

摘要

本账户描述了促进新抗生素发现的基础化学。具体来说,简单羟肟酸衍生物的 NH 酸度促进了新型β-内酰胺(氧马嗪和单环β-内酰胺)、铁摄取限制的铁载体模拟物和细菌靶向的铁载体抗生素(铁载体-抗生素缀合物)的合成。目前有限的抗生素支架的耐药性发展造成了严峻的医疗形势。正如最近所说,“如果你以前没有认真对待抗生素耐药性问题,现在是开始重视的时候了。”英国政府委托的一个项目(https://amr-review.org/)发布了抗生素耐药性在不久的将来对全球造成的影响的估计,其严重程度和规模令人震惊:每年有 1000 万人死亡,国民生产总值至少损失 100 万亿美元。2020 年的 COVID 大流行证实,传染病问题不再局限于局部地区,而是全球性的。许多经典抗生素,尤其是β-内酰胺类抗生素,以前提供了经济有效的治疗方法,但抗生素破坏酶(即β-内酰胺酶)、外排泵和细菌细胞壁通透性屏障的进化使许多类型的细菌,特别是革兰氏阴性菌,产生了耐药性。尽管如此,与其他疗法不同的是,公众期望任何新抗生素都必须便宜。这就造成了市场限制,导致大多数大制药公司放弃了抗生素研究。为了解决这个重大问题,还有很多工作要做。细菌迫切需要隔离必需的铁,这为新抗生素的开发提供了一个弱点。尽管三价铁极其不溶,但细菌的生长和毒力需要毫摩尔浓度的细胞内铁。为此,它们生物合成铁载体(希腊语:iron bearer)并将其分泌到环境中,在环境中它们与铁以高亲和力结合。铁复合物被特定的外膜转运蛋白识别,一旦被主动内化,铁就被释放用于必需的过程。为了节约生物合成能量,一些细菌识别并利用来自竞争菌株的铁载体。作为对这场永无止境的生存斗争的反击,细菌还进化出了铁载体抗生素,即对流氓细菌具有致命作用的铁载体-弹头缀合物。虽然目前没有一种被用于治疗,但天然的铁载体抗生素称为 albomycins 已在临床上使用,其他抗生素在动物感染模型中也表现出良好的耐受性和活性。本文描述了用上述广义结构(铁载体-连接子-药物)合成新抗生素和人工铁载体抗生素的实用方法。利用基于分子识别的铁载体/铁载体抗生素细菌吸收过程,可以设计广谱和高度特异(靶向)的铁载体抗生素,甚至可以重新利用较老或更经典的抗生素。相关的微生物学检测、动物感染研究以及最近 FDA 对头孢地尔的批准证明了它们的有效性。

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