School of Chemical and Biomolecular Engineering, Georgia Institute of Technology, Atlanta, GA, USA.
J Control Release. 2013 Mar 10;166(2):159-71. doi: 10.1016/j.jconrel.2012.12.002. Epub 2012 Dec 13.
Immunization using a microneedle patch coated with vaccine offers the promise of simplified vaccination logistics and increased vaccine immunogenicity. This study examined the stability of influenza vaccine during the microneedle coating process, with a focus on the role of coating formulation excipients. Thick, uniform coatings were obtained using coating formulations containing a viscosity enhancer and surfactant, but these formulations retained little functional vaccine hemagglutinin (HA) activity after coating. Vaccine coating in a trehalose-only formulation retained about 40-50% of vaccine activity, which is a significant improvement. The partial viral activity loss observed in the trehalose-only formulation was hypothesized to come from osmotic pressure-induced vaccine destabilization. We found that inclusion of a viscosity enhancer, carboxymethyl cellulose, overcame this effect and retained full vaccine activity on both washed and plasma-cleaned titanium surfaces. The addition of polymeric surfactant, Lutrol® micro 68, to the trehalose formulation generated phase transformations of the vaccine coating, such as crystallization and phase separation, which was correlated to additional vaccine activity loss, especially when coating on hydrophilic, plasma-cleaned titanium. Again, the addition of a viscosity enhancer suppressed the surfactant-induced phase transformations during drying, which was confirmed by in vivo assessment of antibody response and survival rate after immunization in mice. We conclude that trehalose and a viscosity enhancer are beneficial coating excipients, but the inclusion of surfactant is detrimental to vaccine stability.
使用涂有疫苗的微针贴剂进行免疫接种有望简化疫苗接种流程并提高疫苗的免疫原性。本研究考察了流感疫苗在微针涂层过程中的稳定性,重点研究了涂层配方赋形剂的作用。使用含有粘度增强剂和表面活性剂的涂层配方可获得厚且均匀的涂层,但这些配方在涂层后几乎保留了很少的功能性疫苗血凝素(HA)活性。仅用海藻糖的疫苗涂层保留了约 40-50%的疫苗活性,这是一个显著的改进。仅用海藻糖的配方中观察到的部分病毒活性损失被假设来自渗透压引起的疫苗不稳定。我们发现,包含粘度增强剂羧甲基纤维素克服了这种效应,并在经过清洗和等离子体清洁的钛表面上保留了全部疫苗活性。将聚合物表面活性剂 Lutrol® micro 68 添加到海藻糖配方中会导致疫苗涂层发生相变,例如结晶和相分离,这与额外的疫苗活性损失有关,尤其是在亲水性等离子体清洁的钛上进行涂层时。同样,在干燥过程中添加粘度增强剂可以抑制表面活性剂引起的相转变,这通过在小鼠中进行体内评估抗体反应和免疫后的存活率得到了证实。我们得出结论,海藻糖和粘度增强剂是有益的涂层赋形剂,但表面活性剂的存在不利于疫苗的稳定性。