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Antimicrobial Activity and Toxicity of the Major Lipopeptide Components of Polymyxin B and Colistin: Last-line Antibiotics against Multidrug-Resistant Gram-negative Bacteria

机译:多粘菌素B和colistin的主要脂肽成分的抗菌活性和毒性:多药耐药革兰氏阴性细菌的最后一道抗生素。

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摘要

Polymyxin B and colistin are currently used as a ‘last-line’ treatment for multidrug-resistant Gram-negative bacteria. However very little is known about the pharmacological differences between polymyxin B1, polymyxin B2, colistin A, colistin B, the major cyclic lipopeptides components present in polymyxin B and colistin products. Here, we report on the in vitro and in vivo antimicrobial activity and toxicity of these major lipopeptide components. All four lipopeptides had comparable MICs (<0.125–4 mg/L) against a panel of clinical Gram-negative isolates. They also had comparable in vivo antimicrobial activity (Δlog10 CFU/mL >-3) and nephrotoxicity (mild to moderate histological damage) in mouse models. However, polymyxin B1 and colistin A showed significantly higher (> 3-fold) in vitro apoptotic effect on human kidney proximal tubular HK-2 cells than polymyxin B2 and colistin B, respectively. Compared to the commercial polymyxin and colistin products, the individual lipopeptide components had slightly more in vivo antimicrobial activity. Our results highlight the need to re-assess pharmacopoeial standards for polymyxins B and colistin and to standardize the composition of the different commercial products of polymyxin antibiotics.
机译:多粘菌素B和粘菌素目前被用作对多药耐药的革兰氏阴性细菌的“最后防线”。然而,关于多粘菌素B1,多粘菌素B2,粘菌素A,粘菌素B,多粘菌素B和粘菌素产物中存在的主要环状脂肽成分之间的药理学差异知之甚少。在这里,我们报告了这些主要脂肽成分的体外和体内抗菌活性和毒性。与四种临床革兰氏阴性分离株相比,所有四种脂肽均具有可比的MIC(<0.125–4 mg / L)。它们在小鼠模型中还具有相当的体内抗菌活性(Δlog10CFU / mL> -3)和肾毒性(轻度至中度组织学损害)。但是,多粘菌素B1和粘菌素A对人肾近端肾小管HK-2细胞的体外凋亡作用均显着高于多粘菌素B2和粘菌素B。与商业上的多粘菌素和大肠粘菌素产品相比,单个脂肽组分在体内的抗菌活性略高。我们的结果表明,有必要重新评估多粘菌素B和粘菌素的药典标准,并使多粘菌素抗生素的不同商业产品的组成标准化。

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