School of Biological Sciences, Victoria University of Wellington, Wellington 6012, New Zealand.
Malaghan Institute of Medical Research, Wellington 6012, New Zealand.
ACS Chem Biol. 2024 Jun 21;19(6):1366-1375. doi: 10.1021/acschembio.4c00214. Epub 2024 Jun 3.
Eliciting an antihapten antibody response to vaccination typically requires the use of constructs where multiple copies of the hapten are covalently attached to a larger carrier molecule. The carrier is required to elicit T cell help via presentation of peptide epitopes on major histocompatibility complex (MHC) class II molecules; as such, attachment to full-sized proteins, alone or in a complex, is generally used to account for the significant MHC diversity in humans. While such carrier-based vaccines have proven extremely successful, particularly in protecting against bacterial diseases, they can be challenging to manufacture, and repeated use can be compromised by pre-existing immunity against the carrier. One approach to reducing these complications is to recruit help from type I natural killer T (NKT) cells, which exhibit limited diversity in their antigen receptors and respond to glycolipid antigens presented by the highly conserved presenting molecule CD1d. Synthetic vaccines for universal use can, therefore, be prepared by conjugating haptens to an NKT cell agonist such as α-galactosylceramide (αGalCer, KRN7000). An additional advantage is that the quality of NKT cell help is sufficient to overcome the need for an extra immune adjuvant. However, while initial studies with αGalCer-hapten conjugate vaccines report strong and rapid antihapten antibody responses, they can fail to generate lasting memory. Here, we show that antibody responses to the hapten 4-hydoxy-3-nitrophenyl acetyl (NP) can be improved through additional attachment of a fusion peptide containing a promiscuous helper T cell epitope (Pan DR epitope, PADRE) that binds diverse MHC class II molecules. Such αGalCer-hapten-peptide tricomponent vaccines generate strong and sustained anti-NP antibody titers with increased hapten affinity compared to vaccines without the helper epitope. The tricomponent vaccine platform is therefore suitable for further exploration in the pursuit of efficacious antihapten immunotherapies.
接种疫苗以诱导针对半抗原的抗体反应通常需要使用构建物,其中多个半抗原通过共价键连接到较大的载体分子上。载体需要通过在主要组织相容性复合物 (MHC) Ⅱ类分子上呈递肽表位来引发 T 细胞帮助;因此,单独或在复合物中附着于全尺寸蛋白质通常用于解释人类中 MHC 的显著多样性。尽管这种基于载体的疫苗已被证明非常成功,特别是在预防细菌疾病方面,但它们的制造具有挑战性,并且由于对载体的预先存在的免疫,重复使用可能会受到影响。减少这些并发症的一种方法是从 I 型自然杀伤 T (NKT) 细胞中招募帮助,这些细胞在其抗原受体中表现出有限的多样性,并对由高度保守的呈递分子 CD1d 呈递的糖脂抗原做出反应。因此,可以通过将半抗原与 NKT 细胞激动剂(如α-半乳糖神经酰胺 (αGalCer,KRN7000)偶联来制备通用的合成疫苗。另一个优点是,NKT 细胞帮助的质量足以克服对额外免疫佐剂的需求。然而,虽然最初的αGalCer-半抗原缀合物疫苗研究报告了强烈和快速的抗半抗原抗体反应,但它们可能无法产生持久的记忆。在这里,我们表明,通过附加包含混杂辅助 T 细胞表位 (Pan DR 表位,PADRE)的融合肽,可以改善对半抗原 4-羟基-3-硝基苯乙酰基 (NP)的抗体反应,该表位与多种 MHC Ⅱ类分子结合。与没有辅助表位的疫苗相比,这种αGalCer-半抗原-肽三元疫苗产生了更强和更持久的抗-NP 抗体滴度,并且对半抗原的亲和力增加。因此,三元疫苗平台适合进一步探索有效的抗半抗原免疫疗法。
