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Development of a Highly Thermostable Adjuvanted Human Papillomavirus Vaccine

机译:高度耐热的佐剂人乳头瘤病毒疫苗的研制

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摘要

A major impediment to economical, worldwide vaccine distribution is the requirement for a “cold chain” to preserve antigenicity. We addressed this problem using a model human papillomavirus (HPV) vaccine stabilized by immobilizing HPV16 L1 capsomeres, i.e., pentameric subunits of the virus capsid, within organic glasses formed by lyophilization. Lyophilized glass and liquid vaccine formulations were incubated at 50°C for 12 weeks, and then analyzed for retention of capsomere conformational integrity and the ability to elicit neutralizing antibody responses after immunization of BALB/c mice. Capsomeres in glassy-state vaccines retained tertiary and quaternary structure, and critical conformational epitopes. Moreover, glassy formulations adjuvanted with aluminum hydroxide or aluminum hydroxide and glycopyranoside lipid A were not only as immunogenic as the commercially available HPV vaccine Cervarix®, but also retained complete neutralizing immunogenicity after high-temperature storage. The thermal stability of such adjuvanted vaccine powder preparations may thus eliminate the need for the cold chain.
机译:经济的,全球范围内的疫苗分配的主要障碍是需要“冷链”来保持抗原性。我们使用通过冻干形成的有机玻璃中固定HPV16 L1衣壳即病毒衣壳的五聚体亚基而稳定化的模型人乳头瘤病毒(HPV)疫苗解决了这个问题。将冻干的玻璃和液体疫苗制剂在50°C孵育12周,然后在免疫BALB / c小鼠后分析其帽体构象完整性的保留以及引发中和抗体反应的能力。玻璃态疫苗中的Capsomeres保留了三级和四级结构以及关键的构象表位。此外,佐以氢氧化铝或氢氧化铝和吡喃葡萄糖苷脂质A的玻璃状制剂不仅具有与市售HPV疫苗一样的免疫原性,而且在高温保存后仍具有完全中和的免疫原性。这样的佐剂疫苗粉末制剂的热稳定性可以消除对冷链的需要。

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