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具有强效抗菌活性且肾细胞毒性降低的半合成多粘菌素。

Semisynthetic polymyxins with potent antibacterial activity and reduced kidney cell toxicity.

作者信息

Slingerland Cornelis J, Lysenko Vladyslav, Chaudhuri Samhita, Wesseling Charlotte M J, Barnes Devon, Masereeuw Rosalinde, Martin Nathaniel I

机构信息

Biological Chemistry Group, Institute of Biology Leiden, Leiden University Sylviusweg 72 2333 BE Leiden The Netherlands

Division of Pharmacology, Utrecht Institute of Pharmaceutical Sciences, Utrecht University 3584 CG Utrecht The Netherlands.

出版信息

RSC Med Chem. 2023 Oct 10;14(11):2417-2425. doi: 10.1039/d3md00456b. eCollection 2023 Nov 15.

Abstract

The growing incidence of infections caused by multi-drug resistant Gram-negative bacteria has led to an increased use of last-resort antibiotics such as the polymyxins. Polymyxin therapy is limited by toxicity concerns, most notably nephrotoxicity. Recently we reported the development of a novel class of semisynthetic polymyxins with reduced toxicity wherein the N-terminal lipid and diaminobutyric acid residue are replaced by a cysteine-linked lipid featuring a reductively labile disulfide bond. In the present study we further explored the potential of this approach by also varying the amino acid residue directly adjacent to the polymyxin macrocycle. This led to the identification of new semisynthetic polymyxins that maintain the potent antibacterial activity of the clinically used polymyxin B while exhibiting a further reduction in toxicity toward human proximal tubule epithelial cells. Furthermore, these new polymyxins were found to effectively synergize with novobiocin, rifampicin, and erythromycin against -positive, polymyxin resistant .

摘要

多重耐药革兰氏阴性菌引起的感染发生率不断上升,导致多粘菌素等最后手段抗生素的使用增加。多粘菌素治疗受到毒性问题的限制,最显著的是肾毒性。最近我们报道了一类新型半合成多粘菌素的开发,其毒性降低,其中N端脂质和二氨基丁酸残基被具有还原性不稳定二硫键的半胱氨酸连接脂质取代。在本研究中,我们还通过改变与多粘菌素大环直接相邻的氨基酸残基,进一步探索了这种方法的潜力。这导致鉴定出了新的半合成多粘菌素,它们保持了临床使用的多粘菌素B的强效抗菌活性,同时对人近端肾小管上皮细胞的毒性进一步降低。此外,发现这些新的多粘菌素与新生霉素、利福平及红霉素对革兰氏阳性、耐多粘菌素菌有效协同作用。

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引用本文的文献

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本文引用的文献

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Are outer-membrane targets the solution for MDR Gram-negative bacteria?外膜靶点是否是治疗多重耐药革兰氏阴性菌的方法?
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Antibiotic development - economic, regulatory and societal challenges.抗生素研发——经济、监管及社会挑战
Nat Rev Microbiol. 2020 May;18(5):267-274. doi: 10.1038/s41579-019-0293-3. Epub 2019 Nov 19.

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