早期接种mRNA疫苗后,佐剂重组SARS-CoV-2刺突蛋白疫苗的免疫原性。
Immunogenicity of adjuvanted recombinant SARS-CoV-2 spike protein vaccine after earlier mRNA vaccine doses.
作者信息
Adelglass Jeffrey M, Bradley Paul, Cai Miranda R, Chau Gordon, Kalkeri Raj, Cloney-Clark Shane, Zhu Mingzhu, Cai Zhaohui, Eickhoff Mark, Plested Joyce S, Mallory Raburn M, Dunkle Lisa M
机构信息
Research Your Health, Plano, Tex.
Meridian Clinical Research, Savannah, Ga.
出版信息
J Allergy Clin Immunol. 2025 Jun;155(6):2063-2074.e6. doi: 10.1016/j.jaci.2025.03.015. Epub 2025 Mar 26.
BACKGROUND
To support heterologous vaccine regimens, periodic severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) revaccination requires immunogenicity and safety data for adjuvanted protein-based vaccines following prior mRNA doses.
OBJECTIVE
We sought to assess noninferiority of neutralizing antibody (nAb) titers following a second dose versus a first dose (in a prior study) of an SARS-CoV-2 protein-based vaccine (NVX-CoV2373) administered following a primary series (2 or 3 doses) of an mRNA vaccine.
METHODS
This phase 3, open-label study (2019nCoV-312/NCT05875701) enrolled participants who had received 1 dose of the ancestral SARS-CoV-2 protein-based vaccine in an earlier study (2019nCoV-307/NCT05463068) after a primary series (2 or 3 doses) of a commercial mRNA vaccine. In the current study, participants received an additional dose of protein vaccine (ancestral [n = 104] or Omicron BA.5 [n = 40]) at least 180 days after their previous study dose.
RESULTS
The study enrolled 144 participants. The ratio of anti-Wuhan nAbs (geometric mean titer) at day 28 after this study dose (ancestral 393.2 IU/mL [95% CI 318.0-468.2]) versus previous study dose (396.6 IU/mL [95% CI 328.7-478.6]) was 1.0 (0.8-1.2), meeting noninferiority. The seroresponse rate difference between doses was 7.4% (95% CI -1.2% to 16.5%), also meeting noninferiority. Omicron BA.5 nAb titers suggest cross-protection against emerging variants. The anti-Wuhan nAb ratio at day 28 between Omicron BA.5 vaccine dose in this study (835.0 [597.1-1167.6]) versus the ancestral vaccine in the previous study (436.0 [305.6-622.2]) was 1.9 (1.5-2.5), exceeding superiority criterion. Local and systemic reactions were similar between doses and strains in both studies.
CONCLUSION
A heterologous regimen of 2 adjuvanted, recombinant spike protein vaccine doses following multiple mRNA vaccine doses produced robust immune responses, exhibiting cross-reactivity to some newer variants.
背景
为支持异源疫苗接种方案,在先前接种mRNA剂量后,定期进行严重急性呼吸综合征冠状病毒2(SARS-CoV-2)再次接种需要基于佐剂蛋白的疫苗的免疫原性和安全性数据。
目的
我们试图评估在初次系列(2或3剂)mRNA疫苗接种后接种一剂SARS-CoV-2蛋白疫苗(NVX-CoV2373),第二剂与第一剂(在先前研究中)接种后中和抗体(nAb)滴度的非劣效性。
方法
这项3期开放标签研究(2019nCoV-312/NCT05875701)招募了在先前研究(2019nCoV-307/NCT05463068)中在商业mRNA疫苗的初次系列(2或3剂)接种后接种过1剂原始SARS-CoV-2蛋白疫苗的参与者。在当前研究中,参与者在其先前研究剂量后至少180天接受额外一剂蛋白疫苗(原始株[n = 104]或奥密克戎BA.5[n = 40])。
结果
该研究招募了144名参与者。本次研究剂量(原始株393.2 IU/mL[95%CI 318.0 - 468.2])接种后第28天的抗武汉nAb(几何平均滴度)与先前研究剂量(396.6 IU/mL[95%CI 328.7 - 478.6])的比值为1.0(0.8 - 1.2),符合非劣效性标准。各剂量之间的血清反应率差异为7.4%(95%CI -1.2%至16.5%),也符合非劣效性标准。奥密克戎BA.5 nAb滴度表明对新出现的变异株具有交叉保护作用。本研究中奥密克戎BA.5疫苗剂量接种后第28天的抗武汉nAb比值(835.0[597.1 - 1167.6])与先前研究中原始疫苗(436.0[305.6 - 622.2])的比值为1.9(1.5 - 2.5),超过优效性标准。两项研究中各剂量和毒株之间的局部和全身反应相似。
结论
在多剂mRNA疫苗接种后接种2剂佐剂重组刺突蛋白疫苗的异源接种方案产生了强大的免疫反应,对一些较新的变异株表现出交叉反应性。
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