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Adjuvant formulation structure and composition are critical for the development of an effective vaccine against tuberculosis

机译:佐剂的结构和组成对于开发有效的抗结核疫苗至关重要

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摘要

One third of the world is infected with Mycobacterium tuberculosis (Mtb) with eight million new cases of active tuberculosis (TB) each year. Development of a new vaccine to augment or replace the only approved TB vaccine, BCG, is needed to control this disease. Mtb infection is primarily controlled by TH1 cells through the production of IFN-γ and TNF which activate infected macrophages to kill the bacterium. Here we examine an array of adjuvant formulations containing the TLR4 agonist GLA to identify candidate adjuvants to pair with ID93, a lead TB vaccine antigen, to elicit protective TH1 responses. We evaluate a variety of adjuvant formulations including alum, liposomes, and oil-in-water emulsions to determine how changes in formulation composition alter adjuvant activity. We find that alum and an aqueous nanosuspension of GLA synergize to enhance generation of ID93-specific TH1 responses, whereas neither on their own are effective adjuvants for generation of ID93-specific TH1 responses. For GLA containing oil-in-water emulsions, the selection of the oil component is critical for adjuvant activity, whereas a variety of lipid components may be used in liposomal formulations of GLA. The composition of the liposome formulation of ID93/GLA does alter the magnitude of the TH1 response. These results demonstrate that there are multiple solutions for an effective formulation of a novel TB vaccine candidate that enhances both TH1 generation and protective efficacy.
机译:全世界三分之一的人感染了结核分枝杆菌(Mtb),每年有800万新的活动性结核病(TB)病例。需要开发一种新的疫苗来增加或替代唯一批准的结核病疫苗BCG,以控制这种疾病。 Mtb感染主要由TH1细胞通过产生IFN-γ和TNF来控制,它们激活被感染的巨噬细胞以杀死细菌。在这里,我们检查了一系列含有TLR4激动剂GLA的佐剂制剂,以鉴定与ID93(一种主要的TB疫苗抗原)配对的候选佐剂,以引起保护性TH1应答。我们评估了各种佐剂制剂,包括明矾,脂质体和水包油乳剂,以确定制剂组成的变化如何改变佐剂活性。我们发现明矾和GLA的水性纳米悬浮液协同作用以增强ID93特异性TH1反应的产生,而它们本身都不是产生ID93特异性TH1反应的有效佐剂。对于含有GLA的水包油乳液,油成分的选择对于佐剂活性至关重要,而GLA脂质体制剂中可以使用多种脂质成分。 ID93 / GLA脂质体制剂的组成确实会改变TH1反应的幅度。这些结果表明,有多种解决方案可有效配制可提高TH1产生和保护功效的新型TB候选疫苗。

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