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一种含2-氨基恶唑的新型杀菌性氯化衍生物可增强黏菌素对多重耐药鲍曼不动杆菌的抗菌作用。

A new bactericidal chlorinated derivative containing 2-aminooxazole potentiates antibacterial action of colistin against multidrug-resistant acinetobacter baumannii.

作者信息

Diepoltová Adéla, Nawrot Daria Elzbieta, Janďourek Ondřej, Juhás Martin, Bárta Pavel, Vávrová Pavlína, Pallabothula Vinod Sukanth Kumar, Dudášová-Hatoková Paulína, Vejsová Marcela, Voxová Barbora, Österreicher Jan, Štěrbová-Kovaříková Petra, Nachtigal Petr, Zitko Jan, Konečná Klára

机构信息

Faculty of Pharmacy in Hradec Králové, Charles University, Akademika Heyrovského 1203, 500 03, Hradec Králové, Czech Republic.

Department of Chemistry, Faculty of Science, University of Hradec Králové, Rokitanského 62, 500 03, Hradec Králové III, Czech Republic.

出版信息

Med Microbiol Immunol. 2025 Sep 19;214(1):44. doi: 10.1007/s00430-025-00854-y.

Abstract

This comprehensive study provides insight into the antibacterial action of a recently published 2-chloro-N-(oxazol-2-yl)isonicotinamide (AB15), intending to assess its potential as a candidate adjuvant molecule to support existing antibacterial drugs. Within the determination of the antibacterial effect, a promising activity against a member of the ESKAPE group with reduced treatment options, biofilm producer, Acinetobacter baumannii, was recognized (MIC of AB15 ranged from 15.63 to 62.5 µM). In addition, AB15 exhibited bactericidal activity and non/low-toxicity in vitro (IC > 1000 µM using HK-2 cells) and in vivo (LD > 500 mg/kg of body weight of the Galleria mellonella larvae, for both intra-hemocoel and per oral administration routes). Checkerboard assay revealed additive and synergistic interactions of AB15 and last-resort antibiotic drug, colistin (CST). Moreover, attention was also given to a frequently overlooked antibiofilm activity - the ability to suppress bacterial dissemination from microbial biofilms, and parameter MBDC (minimum biofilm dissemination concentration) was introduced. The study of the antibiofilm activity of AB15 and CST, both acting individually, or in AB15 + CST combination, revealed that AB15 has significant potential to suppress bacterial dissemination from biofilm formed by a clinical isolate Acinetobacter baumannii and that it contributes to this effect when combined with CST. Finally, AB15 + CST combination demonstrated significantly greater biocompatibility towards human erythrocytes than CST acting individually at an equivalent antibiofilm-effective concentration. The role of AB15 as a promising adjuvant molecule to CST is also supported by its distinct mechanism of action, which reduces the risk of antimicrobial resistance emergence. To conclude, AB15 exhibits several essential attributes that support its designation as a promising antibiotic adjuvant.

摘要

这项综合性研究深入探讨了最近发表的2-氯-N-(恶唑-2-基)异烟酰胺(AB15)的抗菌作用,旨在评估其作为辅助现有抗菌药物的候选分子的潜力。在确定抗菌效果时,发现AB15对治疗选择有限的ESKAPE组中的一员、生物膜产生菌鲍曼不动杆菌具有良好的活性(AB15的MIC范围为15.63至62.5μM)。此外,AB15在体外(使用HK-2细胞时IC>1000μM)和体内(对于血腔注射和口服给药途径,大蜡螟幼虫的体重LD>500mg/kg)均表现出杀菌活性和无/低毒性。棋盘法揭示了AB15与最后手段抗生素药物粘菌素(CST)的相加和协同相互作用。此外,还关注了一个经常被忽视的抗生物膜活性——抑制细菌从微生物生物膜中扩散的能力,并引入了参数MBDC(最小生物膜扩散浓度)。对AB15和CST单独或联合使用时的抗生物膜活性研究表明,AB15具有显著的潜力抑制临床分离的鲍曼不动杆菌形成的生物膜中的细菌扩散,并且与CST联合使用时有助于这种效果。最后,在等效的抗生物膜有效浓度下,AB15+CST组合对人红细胞的生物相容性明显高于单独使用的CST。AB15作为CST的有前景的辅助分子的作用也得到了其独特作用机制的支持,该机制降低了抗菌耐药性出现的风险。总之,AB15表现出几个基本属性,支持其被指定为有前景的抗生素佐剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b486/12449380/1fea35099f3f/430_2025_854_Fig1_HTML.jpg

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