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弹性蛋白样多肽掺入热敏感脂质体改善对抗肌肉骨骼细菌病原体的抗生素治疗。

Elastin-like polypeptide incorporated thermally sensitive liposome improve antibiotic therapy against musculoskeletal bacterial pathogens.

机构信息

a Center for Veterinary Health Sciences , Oklahoma State University , Stillwater , OK , USA.

出版信息

Int J Hyperthermia. 2018 Mar;34(2):201-208. doi: 10.1080/02656736.2017.1420249.

Abstract

Musculoskeletal infections caused by bacteria such as Staphylococcus aureus and Pseudomonas aeruginosa in children and adults can lead to adverse outcomes including a need for extensive surgical debridement and limb amputation. To enable targeted antimicrobial release in infected tissues, the objective of this study was to design and investigate novel elastin-like polypeptide (ELP)-based thermally sensitive liposomes in vitro. ELP biopolymers can change their phase behaviour at higher temperatures. We hypothesised that ELP-TSL will improve therapeutic efficacy by releasing antimicrobial payloads locally at higher temperatures (≥39 °C). ELP-TSL library were formulated by varying cholesterol and phospholipid composition by the thin film and extrusion method. A broad-spectrum antimicrobial (Ciprofloxacin or Cipro) was encapsulated inside the liposomes by the ammonium sulphate gradient method. Cipro release from ELP-TSLs was assessed in physiological buffers containing ∼25% serum by fluorescence spectroscopy, and efficacy against Staphylococcus aureus and Pseudomonas aeruginosa was assessed by disc diffusion and planktonic assay. Active loading of Cipro achieved an encapsulation efficiency of 40-70% in the ELP-TSL depending upon composition. ELP-TSL Cipro release was near complete at ≥39 °C; however, the release rates could be delayed by cholesterol. Triggered release of Cipro from ELP-TSL at ∼42 °C induced significant killing of S. aureus and P. aeruginosa compared to 37 °C. Our in vitro data suggest that ELP-TSL may potentially improve bacterial wound therapy in patients.

摘要

金黄色葡萄球菌和铜绿假单胞菌等细菌引起的儿童和成人肌肉骨骼感染可导致不良后果,包括需要广泛的清创和截肢。为了在感染组织中实现靶向抗菌药物释放,本研究旨在设计和研究新型弹性蛋白样多肽(ELP)基热敏脂质体的体外性能。ELP 生物聚合物在较高温度下可以改变其相行为。我们假设 ELP-TSL 将通过在较高温度(≥39°C)局部释放抗菌有效负载来提高治疗效果。ELP-TSL 库通过薄膜和挤出法改变胆固醇和磷脂组成来进行配方设计。通过硫酸铵梯度法将广谱抗菌药物(环丙沙星或 Cipro)封装在脂质体中。通过荧光光谱法在含有约 25%血清的生理缓冲液中评估 Cipro 的释放情况,并通过碟扩散和浮游生物测定评估其对金黄色葡萄球菌和铜绿假单胞菌的疗效。根据组成的不同,ELP-TSL 中 Cipro 的主动负载可实现 40-70%的包封效率。ELP-TSL 中 Cipro 的释放在≥39°C 时接近完全,但胆固醇可延迟释放速率。与 37°C 相比,ELP-TSL 在约 42°C 时触发 Cipro 的释放可显著杀死金黄色葡萄球菌和铜绿假单胞菌。我们的体外数据表明,ELP-TSL 可能有望改善患者的细菌伤口治疗效果。

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