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首页> 外文期刊>International Journal of Nanomedicine >Development of a thermostable nanoemulsion adjuvanted vaccine against tuberculosis using a design-of-experiments approach
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Development of a thermostable nanoemulsion adjuvanted vaccine against tuberculosis using a design-of-experiments approach

机译:使用实验设计方法开发抗结核的热稳定纳米乳剂佐剂疫苗

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Background: Adjuvants have the potential to increase the efficacy of protein-based vaccines but need to be maintained within specific temperature and storage conditions. Lyophilization can be used to increase the thermostability of protein pharmaceuticals; however, no marketed vaccine that contains an adjuvant is currently lyophilized, and lyophilization of oil-in-water nanoemulsion adjuvants presents a specific challenge. We have previously demonstrated the feasibility of lyophilizing a candidate adjuvanted protein vaccine against Mycobacterium tuberculosis ( Mtb ), ID93 + GLA-SE, and the subsequent improvement of thermostability; however, further development is required to prevent physicochemical changes and degradation of the TLR4 agonist glucopyranosyl lipid adjuvant formulated in an oil-in-water nanoemulsion (SE). Materials and methods: In this study, we took a systematic approach to the development of a thermostable product by first identifying compatible solution conditions and stabilizing excipients for both antigen and adjuvant. Next, we applied a design-of-experiments approach to identify stable lyophilized drug product formulations. Results: We identified specific formulations that contain disaccharide or a combination of disaccharide and mannitol that can achieve substantially improved thermostability and maintain immunogenicity in a mouse model when tested in accelerated and real-time stability studies. Conclusion: These efforts will aid in the development of a platform formulation for use with other similar vaccines.
机译:背景:佐剂有可能提高基于蛋白质的疫苗的功效,但需要保持在特定的温度和储存条件下。冻干可用于提高蛋白质药物的热稳定性;然而,目前尚无冻干市售的含有佐剂的疫苗,而水包油纳米乳剂佐剂的冻干提出了特殊的挑战。我们先前已经证明了冻干针对结核分枝杆菌(Mtb),ID93 + GLA-SE的候选佐剂蛋白疫苗的可行性,以及随后改善的热稳定性;但是,需要进一步开发以防止在水包油纳米乳剂(SE)中配制的TLR4激动剂吡喃葡萄糖基脂质佐剂的理化变化和降解。材料和方法:在这项研究中,我们通过首先确定相容的溶液条件并稳定了抗原和佐剂的赋形剂,采用了系统方法来开发热稳定的产品。接下来,我们应用了实验设计方法来确定稳定的冻干药物产品配方。结果:我们鉴定了包含二糖或二糖和甘露醇的组合的特定配方,当在加速和实时稳定性研究中进行测试时,它们可以在小鼠模型中显着提高热稳定性并保持免疫原性。结论:这些努力将有助于开发与其他类似疫苗一起使用的平台制剂。

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