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多粘菌素 B 缀合物与不同性质的仿生合成聚合物。

Polymyxin B Conjugates with Bio-Inspired Synthetic Polymers of Different Nature.

机构信息

Institute of Chemistry, Saint-Petersburg State University, 198504 St. Petersburg, Russia.

Institute of Macromolecular Compounds, Russian Academy of Sciences, 199004 St. Petersburg, Russia.

出版信息

Int J Mol Sci. 2023 Jan 17;24(3):1832. doi: 10.3390/ijms24031832.

Abstract

The emergence and growth of bacterial resistance to antibiotics poses an enormous threat to humanity in the future. In this regard, the discovery of new antibiotics and the improvement of existing ones is a priority task. In this study, we proposed the synthesis of new polymeric conjugates of polymyxin B, which is a clinically approved but limited-use peptide antibiotic. In particular, three carboxylate-bearing polymers and one synthetic glycopolymer were selected for conjugation with polymyxin B (PMX B), namely, poly(α,L-glutamic acid) (PGlu), copolymer of L-glutamic acid and L-phenylalanine (P(Glu--Phe)), copolymer of N-vinyl succinamic acid and N-vinylsuccinimide (P(VSAA--VSI)), and poly(2-deoxy-2-methacrylamido-D-glucose) (PMAG). Unlike PGlu and PMAG, P(Glu--Phe) and P(VSAA--VSI) are amphiphilic and form nanoparticles in aqueous media. A number of conjugates with different polymyxin B loading were synthesized and characterized. In addition, the complex conjugates of PGLu or PMAG with polymyxin B and deferoxamine (siderophore) were obtained. A release of PMX B from Schiff base and amide-linked polymer conjugates was studied in model buffer media with pH 7.4 and 5.8. In both cases, a more pronounced release was observed under slightly acidic conditions. The cytotoxicity of free polymers and PMX B as well as their conjugates was examined in human embryonic kidney cells (HEK 293T cell line). All conjugates demonstrated reduced cytotoxicity compared to the free antibiotic. Finally, the antimicrobial efficacy of the conjugates against was determined and compared. The lowest values of minimum inhibitory concentrations (MIC) were observed for polymyxin B and polymyxin B/deferoxamine conjugated with PMAG. Among the polymers tested, PMAG appears to be the most promising carrier for delivery of PMX B in conjugated form due to the good preservation of the antimicrobial properties of PMX B and the ability of controlled drug release.

摘要

细菌对抗生素的耐药性的出现和增长对未来的人类构成了巨大威胁。在这方面,发现新的抗生素并改进现有的抗生素是当务之急。在这项研究中,我们提出了合成新的多粘菌素 B 聚合物缀合物的方法,多粘菌素 B 是一种临床批准但使用有限的肽类抗生素。特别是,选择了三种带有羧酸盐的聚合物和一种合成糖聚合物与多粘菌素 B(PMX B)缀合,即聚(α,L-谷氨酸)(PGlu)、L-谷氨酸和 L-苯丙氨酸的共聚物(P(Glu--Phe))、N-乙烯基琥珀酰胺酸和 N-乙烯基琥珀酰亚胺的共聚物(P(VSAA--VSI))和聚(2-脱氧-2-甲酰胺基-D-葡萄糖)(PMAG)。与 PGlu 和 PMAG 不同,P(Glu--Phe)和 P(VSAA--VSI)是两亲性的,并在水介质中形成纳米粒子。合成了具有不同多粘菌素 B 载量的多种缀合物并进行了表征。此外,还获得了 PGLu 或 PMAG 与多粘菌素 B 和去铁胺(铁载体)的复合物缀合物。在 pH 值为 7.4 和 5.8 的模型缓冲介质中研究了席夫碱和酰胺键连接的聚合物缀合物中 PMX B 的释放。在这两种情况下,在略酸性条件下观察到更明显的释放。在人胚肾细胞(HEK 293T 细胞系)中研究了游离聚合物和 PMX B 及其缀合物的细胞毒性。与游离抗生素相比,所有缀合物的细胞毒性均降低。最后,测定了缀合物对的抗菌功效并进行了比较。观察到最低的最小抑菌浓度(MIC)值是多粘菌素 B 和与 PMAG 缀合的多粘菌素 B/去铁胺。在所测试的聚合物中,PMAG 似乎是递送 PMX B 缀合物的最有前途的载体,因为它能很好地保持 PMX B 的抗菌性能和控制药物释放的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f14/9915011/4a2824a91742/ijms-24-01832-g001.jpg

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