Biryukov Sergei S, Rasley Amy, Davies Michael L, Klimko Christopher P, Dankmeyer Jennifer L, Hunter Melissa, Rill Nathaniel O, Shoe Jennifer L, Miller Jeremy, Talyansky Yuli, Sullinger Barbara, Herrera Matheo, Huang Daniel, Bautista Leslie, Pepe Lucy, Peters Sandra K G, Xander Christian J, Martinez Elsie E, Toothman Ronald G, Mlynek Kevin D, Bozue Joel A, Qiu Ju, Fischer Nicholas O, Cote Christopher K
Bacteriology Division, United States Army Medical Research Institute of Infectious Diseases, Frederick, MD, United States.
Biosciences and Biotechnology Division, Lawrence Livermore National Laboratory, Livermore, CA, United States.
Front Immunol. 2025 Jun 26;16:1603710. doi: 10.3389/fimmu.2025.1603710. eCollection 2025.
is the etiological agent of plague, a disease that remains a concern as demonstrated by recent outbreaks in Madagascar. Infection with results in a rapidly progressing illness that can only be successfully treated with antibiotics given shortly after symptom onset. Live attenuated or whole cell inactivated vaccines confer protection against bubonic plague, but pneumonic plague has been more difficult to prevent. Novel effective subunit vaccine formulations may circumvent some of these shortfalls. Here, we compare the immunogenicity generated by an advanced subunit vaccine (F1V fusion protein) and a nanolipoprotein particle (NLP)-based vaccine.
The NLP, a high-density lipoprotein mimetic, provides a nanoscale delivery platform for recombinant antigens LcrV (V) and F1. BALB/c mice were immunized via subcutaneous injection twice, three or four weeks apart. Four weeks later, splenocytes and sera were collected for immune profiling, and mice were challenged with aerosolized CO92.
Both formulations induced a strong IgG response against the F1 and V proteins, along with a robust memory B cell response and a balanced cell-mediated immune response as evidenced by both Th1- and Th2-related cytokines. The NLP-based vaccine induced a stronger cytokine response against F1, V, and F1V proteins relative to the F1V vaccine. As with F1V, the inclusion of Alhydrogel (Alu) in NLP vaccine formulations was critical for enhanced immunogenicity and protective efficacy. Mice that received two doses of F1:V:NLP + Alu and CpG were completely protected from a challenge with approximately eight median lethal doses of aerosolized CO92 and this protection confirmed the well-documented synergy between the F1 and V antigens in context of pneumonic plague. The NLPs have defined regions of polarity that facilitates the incorporation of a wide range of adjuvants and antigens with distinct physicochemical properties and are an excellent candidate platform for the development of multi-antigen vaccines.
鼠疫耶尔森菌是鼠疫的病原体,近期马达加斯加的疫情爆发表明,这种疾病仍然令人担忧。感染鼠疫耶尔森菌会导致病情迅速发展,只有在症状出现后不久给予抗生素才能成功治疗。减毒活疫苗或全细胞灭活疫苗可提供针对腺鼠疫的保护,但预防肺鼠疫则更加困难。新型有效的亚单位疫苗制剂可能会规避其中一些不足。在此,我们比较了一种先进的亚单位疫苗(F1V融合蛋白)和一种基于纳米脂蛋白颗粒(NLP)的疫苗所产生的免疫原性。
NLP是一种高密度脂蛋白模拟物,为重组鼠疫耶尔森菌抗原LcrV(V)和F1提供纳米级递送平台。通过皮下注射对BALB/c小鼠进行两次免疫,间隔三或四周。四周后,收集脾细胞和血清进行免疫分析,并对小鼠进行雾化鼠疫耶尔森菌CO92攻击。
两种制剂均诱导了针对F1和V蛋白的强烈IgG反应,以及强大的记忆B细胞反应和平衡的细胞介导免疫反应,Th1和Th2相关细胞因子均证明了这一点。相对于F1V疫苗,基于NLP的疫苗诱导了针对F1、V和F1V蛋白更强的细胞因子反应。与F1V一样,在NLP疫苗制剂中加入氢氧化铝(Alu)对于增强免疫原性和保护效力至关重要。接受两剂F1:V:NLP + Alu和CpG的小鼠完全受到保护,免受约八个雾化鼠疫耶尔森菌CO92半数致死剂量攻击,这种保护证实了在肺鼠疫背景下F1和V抗原之间有据可查的协同作用。NLP具有明确的极性区域,便于掺入具有不同物理化学性质的多种佐剂和抗原,是开发多抗原疫苗的优秀候选平台。
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