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Formulation of carbapenems loaded gold nanoparticles to combat multi-antibiotic bacterial resistance: In vitro antibacterial study

机译:配制碳青霉烯负载金纳米粒子,用于打击多抗生素细菌耐药性:体外抗菌研究

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Despite the fact that carbapenems (powerful beta-lactams antibiotics) were able to fight serious infectious diseases, nowadays the spread of carbapenems-resistant bacteria is considered the main challenge in antibacterial therapy. In this study, we focused on evaluating the surface conjugation of carbapenems (imipenem and meropenem) with gold nanoparticles as a delivering strategy to specifically and safely maximize their therapeutic efficacy while destroying the developing resistance of the pathogens. Different particle size formulae (35, 70 and 200 nm) were prepared by citrate reduction method. The prepared nanoparticles were functionalized with imipenem (Ipm) or meropenem (Mem) and physicochemically characterized for loading efficiency, particle size, morphology, and in-vitro release. The antibacterial efficacy was also evaluated against carbapenems resistant Gram-negative bacteria isolated from infected human, through measuring the minimum inhibitory concentration and antibiotic kill test. All the obtained gold nanoparticles showed a distinct nano-size with loading efficiency up to 72% and 74% for Ipm and Mem, respectively. The conjugation and physico-chemical stability of the formulated carbapenems were confirmed by FTIR and X-RPD. Diffusion driven release behavior was observed for both Ipm and Mem from all of the loaded gold nanoparticles. For both Ipm and Mem, formula with 35 nm diameter showed the most significant enhancement in antibacterial activity against all the selected isolates including Klebsiella pneumoniae, Proteus mirabilis and Acinteobacter baumanii. Ipm loaded Gold nanoparticles demonstrated decrease in the MIC of Ipm down to four folds, whereas, Mem loaded gold nanoparticles showed decrease in the MIC of Mem down to three folds on the tested bacterial isolates. Based on these results, the formulation of carbapenems-loaded gold nanoparticles demonstrated to be a promising nano-size delivery vehicle for improving the therapeutic activity and destroying the bacterial resistance for carbapenems. (C) 2017 Elsevier B. V. All rights reserved.
机译:尽管碳青霉素(强大的β-内酰胺抗生素)能够对抗严重的传染病,但是耐鲤鱼抗性细菌的传播被认为是抗菌治疗中的主要挑战。在这项研究中,我们专注于评估Carbapems(ImipeNem和Meropenem)与金纳米颗粒的表面缀合,作为递送策略,以具体和安全地最大化其治疗效果,同时破坏病原体的显影性。通过柠檬酸盐还原法制备不同的粒度配方(35,70和200nm)。将制备的纳米颗粒用亚胺烯(IPM)或MEMOPENEM(MEM)官能化,并物理化学表征用于加载效率,粒度,形态和体外释放。还通过测量最小抑制浓度和抗生素杀灭试验,对耐药革兰阴性细菌进行抗菌疗效进行抗菌疗效。所有得到的金纳米颗粒分别显示出具有较小纳米尺寸,其加载效率高达IPM和MEM的72%和74%。通过FTIR和X-RPD确认配制的肉豆蔻蛋白的缀合和物理化学稳定性。对于来自所有负载的金纳米颗粒的IPM和MEM,观察到扩散驱动释放行为。对于IPM和MEM,具有35nm直径的配方表明,对所有所选分离物的抗菌活性具有最显着的增强,包括Klebsiella Pneumoniae,Proteus mirabilis和Acinteobacter Baumanii。 IPM负载的金纳米颗粒在下降至四倍的IPM的MIC中展示了下降,而MEM载纳米颗粒显示在测试的细菌分离株上的MEM的MIC下降至三倍。基于这些结果,碳植物负载的金纳米粒子的制剂证明是有希望的纳米尺寸输送载体,用于改善治疗活性并破坏碳癌癌的细菌抗性。 (c)2017 Elsevier B. V.保留所有权利。

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