State Key Laboratory for Animal Disease Control and Prevention, Guangdong Laboratory for Lingnan Modern Agriculture, College of Veterinary Medicine, South China Agricultural University, Guangzhou, Guangdong, China.
Key Laboratory of Zoonosis of Ministry of Agricultural and Rural Affairs, Guangdong Provincial Key Laboratory of Veterinary Pharmaceutics Development and Safety Evaluation, Guangzhou, Guangdong, China.
mSystems. 2024 Jun 18;9(6):e0010924. doi: 10.1128/msystems.00109-24. Epub 2024 May 2.
Polymyxin is used as a last resort antibiotics for infections caused by multi-drug resistant (MDR) Gram-negative bacteria and is often combined with other antibiotics to improve clinical effectiveness. However, the synergism of colistin and other antibiotics remains obscure. Here, we revealed a notable synergy between colistin and flavomycin, which was traditionally used as an animal growth promoter and has limited activity against Gram-negative bacteria, using checkerboard assay and time-kill curve analyses. The importance of membrane penetration induced by colistin was assessed by examining the intracellular accumulation of flavomycin and its antimicrobial impact on () strains with truncated lipopolysaccharides. Besides, a mutation in the flavomycin binding site was created to confirm its role in the observed synergy. This synergy is manifested as an augmented penetration of the outer membrane by colistin, leading to increased intracellular accumulation of flavomycin and enhanced cell killing thereafter. The observed synergy was dependent on the antimicrobial activity of flavomycin, as mutation of its binding site abolished the synergy. studies confirmed the efficacy of colistin combined with flavomycin against MDR infections. This study is the first to demonstrate the synergistic effect between colistin and flavomycin, shedding light on their respective roles in this synergism. Therefore, we propose flavomycin as an adjuvant to enhance the potency of colistin against MDR Gram-negative bacteria.
Colistin is a critical antibiotic in combating multi-drug resistant Gram-negative bacteria, but the emergence of mobilized colistin resistance (mcr) undermines its effectiveness. Previous studies have found that colistin can synergy with various drugs; however, its exact mechanisms with hydrophobic drugs are still unrevealed. Generally, the membrane destruction of colistin is thought to be the essential trigger for its interactions with its partner drugs. Here, we use clustered regularly interspaced palindromic repeats (CRISPR)-CRISPR-associated protein 9 (Cas9) for specifically mutating the binding site of one hydrophobic drug (flavomycin) and show that antimicrobial activity of flavomycin is critical for the synergy. Our results first give the evidence that the synergy is set off by colistin's membrane destruction and operated the final antimicrobial function by its partner drugs.
多黏菌素通常被用作治疗多重耐药(MDR)革兰氏阴性菌感染的最后手段抗生素,并且经常与其他抗生素联合使用以提高临床疗效。然而,黏菌素与其他抗生素的协同作用仍不清楚。在这里,我们使用棋盘试验和时间杀伤曲线分析发现,黏菌素和传统上用作动物生长促进剂且对革兰氏阴性菌活性有限的弗氏菌素之间存在显著协同作用。通过检查弗氏菌素的细胞内积累及其对截短脂多糖()菌株的抗菌作用,评估了黏菌素诱导的膜穿透的重要性。此外,创建了弗氏菌素结合位点的突变以确认其在观察到的协同作用中的作用。这种协同作用表现为黏菌素对 外膜的穿透增强,导致弗氏菌素的细胞内积累增加,随后细胞杀伤增强。观察到的协同作用取决于弗氏菌素的抗菌活性,因为其结合位点的突变消除了协同作用。 研究证实黏菌素联合弗氏菌素对抗 MDR 感染的疗效。这项研究首次证明了黏菌素和弗氏菌素之间的协同作用,揭示了它们在这种协同作用中的各自作用。因此,我们建议将弗氏菌素作为增强黏菌素对 MDR 革兰氏阴性菌效力的佐剂。
黏菌素是对抗多药耐药革兰氏阴性菌的关键抗生素,但 Mobilized colistin resistance (mcr) 的出现削弱了其效力。以前的研究发现,黏菌素可以与各种药物协同作用;然而,其与疏水性药物的确切机制仍未得到揭示。通常,认为黏菌素的膜破坏是其与伙伴药物相互作用的必要触发因素。在这里,我们使用成簇规律间隔短回文重复(CRISPR)-CRISPR 相关蛋白 9(Cas9)特异性突变一种疏水性药物(弗氏菌素)的结合位点,并表明弗氏菌素的抗菌活性对于协同作用至关重要。我们的结果首次证明,协同作用是由黏菌素的膜破坏引发的,并通过其伙伴药物发挥最终的抗菌作用。
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