针对刺突蛋白和非刺突蛋白上保守表位的泛 SARS-CoV-2 疫苗,以诱导有效、广谱和持久的免疫应答。
Toward a pan-SARS-CoV-2 vaccine targeting conserved epitopes on spike and non-spike proteins for potent, broad and durable immune responses.
机构信息
UBI Asia, Hsinchu, Taiwan.
StatPlus, Inc., Taipei, Taiwan.
出版信息
PLoS Pathog. 2023 Apr 20;19(4):e1010870. doi: 10.1371/journal.ppat.1010870. eCollection 2023 Apr.
BACKGROUND
The SARS-CoV-2 non-Spike (S) structural protein targets on nucleocapsid (N), membrane (M) and envelope (E), critical in the host cell interferon response and memory T-cell immunity, are grossly overlooked in COVID vaccine development. The current Spike-only vaccines bear an intrinsic shortfall for promotion of a fuller T cell immunity. Vaccines designed to target conserved epitopes could elicit strong cellular immune responses that would synergize with B cell responses and lead to long-term vaccine success. We pursue a universal (pan-SARS-CoV-2) vaccine against Delta, Omicrons and ever-emergent new mutants.
METHODS AND FINDINGS
We explored booster immunogenicity of UB-612, a multitope-vaccine that contains S1-RBD-sFc protein and sequence-conserved promiscuous Th and CTL epitope peptides on the Sarbecovirus N, M and S2 proteins. To a subpopulation (N = 1,478) of infection-free participants (aged 18-85 years) involved in a two-dose Phase-2 trial, a UB-612 booster (third dose) was administered 6-8 months after the second dose. The immunogenicity was evaluated at 14 days post-booster with overall safety monitored until the end of study. The booster induced high viral-neutralizing antibodies against live Wuhan WT (VNT50, 1,711) and Delta (VNT50, 1,282); and against pseudovirus WT (pVNT50, 11,167) vs. Omicron BA.1/BA.2/BA.5 variants (pVNT50, 2,314/1,890/854), respectively. The lower primary neutralizing antibodies in the elderly were uplifted upon boosting to approximately the same high level in young adults. UB-612 also induced potent, durable Th1-oriented (IFN-γ+-) responses (peak/pre-boost/post-boost SFU/106 PBMCs, 374/261/444) along with robust presence of cytotoxic CD8+ T cells (peak/pre-boost/post-boost CD107a+-Granzyme B+, 3.6%/1.8%/1.8%). This UB-612 booster vaccination is safe and well tolerated without SAEs.
CONCLUSIONS
By targeting conserved epitopes on viral S2, M and N proteins, UB-612 could provide potent, broad and long-lasting B-cell and T-cell memory immunity and offers the potential as a universal vaccine to fend off Omicrons and new VoCs without resorting to Omicron-specific immunogens.
TRIAL REGISTRATION
ClinicalTrials.gov ID: NCT04773067; ClinicalTrials.gov ID: NCT05293665; ClinicalTrials.gov ID: NCT05541861.
背景
SARS-CoV-2 的非刺突(S)结构蛋白针对核衣壳(N)、膜(M)和包膜(E),这些蛋白在宿主细胞干扰素反应和记忆 T 细胞免疫中至关重要,但在 COVID 疫苗开发中被严重忽视。目前仅针对 Spike 的疫苗在促进更全面的 T 细胞免疫方面存在固有缺陷。针对保守表位设计的疫苗可以引发强烈的细胞免疫反应,与 B 细胞反应协同作用,并导致长期疫苗成功。我们正在开发一种针对 Delta、Omicron 和不断出现的新突变株的通用(泛 SARS-CoV-2)疫苗。
方法和发现
我们探索了 UB-612 的增强免疫原性,UB-612 是一种多表位疫苗,包含 S1-RBD-sFc 蛋白和 Sarbecovirus N、M 和 S2 蛋白上序列保守的广泛 Th 和 CTL 表位肽。在一项两剂 2 期试验中,对无感染史的参与者(年龄 18-85 岁)的亚组(N=1478)进行 UB-612 加强针(第三剂)接种,在第二剂接种后 6-8 个月进行。在加强针接种后 14 天通过总体安全性监测评估免疫原性,直至研究结束。加强针诱导了针对活武汉 WT(VNT50,1711)和 Delta(VNT50,1282)的高病毒中和抗体;以及针对假病毒 WT(pVNT50,11167)与 Omicron BA.1/BA.2/BA.5 变体(pVNT50,2314/1890/854)的中和抗体。在老年人中,初级中和抗体水平较低,但在加强免疫后,可提升至与年轻人相似的高水平。UB-612 还诱导了强烈的、持久的 Th1 定向(IFN-γ+-)反应(峰值/加强针前/加强针后 SFU/106 PBMCs,374/261/444),同时存在大量的细胞毒性 CD8+T 细胞(峰值/加强针前/加强针后 CD107a+-颗粒酶 B+,3.6%/1.8%/1.8%)。这种 UB-612 加强疫苗接种安全且耐受性良好,无严重不良事件。
结论
通过针对病毒 S2、M 和 N 蛋白上的保守表位,UB-612 可以提供强大、广泛和持久的 B 细胞和 T 细胞记忆免疫,并有可能成为一种通用疫苗,抵御 Omicron 和新的变异株,而无需依赖 Omicron 特异性免疫原。
试验注册
临床试验.gov 标识符:NCT04773067;临床试验.gov 标识符:NCT05293665;临床试验.gov 标识符:NCT05541861。
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