Beavis Ashley C, Li Zhuo, Briggs Kelsey, Huertas-Díaz María Cristina, Wrobel Elizabeth R, Najera Maria, An Dong, Orr-Burks Nichole, Murray Jackelyn, Patil Preetish, Huang Jiachen, Mousa Jarrod, Hao Linhui, Hsiang Tien-Ying, Gale Michael, Harvey Stephen B, Tompkins S Mark, Hogan Robert Jeffrey, Lafontaine Eric R, Jin Hong, He Biao
CyanVac LLC, Athens, Georgia, 30602.
Department of Infectious Diseases, College of Veterinary Medicine, University of Georgia, Athens, Georgia.
bioRxiv. 2022 Jun 8:2022.06.07.495215. doi: 10.1101/2022.06.07.495215.
Immunization with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccines has greatly reduced coronavirus disease 2019 (COVID-19)-related deaths and hospitalizations, but waning immunity and the emergence of variants capable of immune escape indicate the need for novel SARS-CoV-2 vaccines. An intranasal parainfluenza virus 5 (PIV5)-vectored COVID-19 vaccine CVXGA1 has been proven efficacious in animal models and blocks contact transmission of SARS-CoV-2 in ferrets. CVXGA1 vaccine is currently in human clinical trials in the United States. This work investigates the immunogenicity and efficacy of CVXGA1 and other PIV5-vectored vaccines expressing additional antigen SARS-CoV-2 nucleoprotein (N) or SARS-CoV-2 variant spike (S) proteins of beta, delta, gamma, and omicron variants against homologous and heterologous challenges in hamsters. A single intranasal dose of CVXGA1 induces neutralizing antibodies against SARS-CoV-2 WA1 (ancestral), delta variant, and omicron variant and protects against both homologous and heterologous virus challenges. Compared to mRNA COVID-19 vaccine, neutralizing antibody titers induced by CVXGA1 were well-maintained over time. When administered as a boost following two doses of a mRNA COVID-19 vaccine, PIV5-vectored vaccines expressing the S protein from WA1 (CVXGA1), delta, or omicron variants generate higher levels of cross-reactive neutralizing antibodies compared to three doses of a mRNA vaccine. In addition to the S protein, the N protein provides added protection as assessed by the highest body weight gain post-challenge infection. Our data indicates that PIV5-vectored COVID-19 vaccines, such as CVXGA1, can serve as booster vaccines against emerging variants.
接种严重急性呼吸综合征冠状病毒2(SARS-CoV-2)疫苗已大幅降低了2019冠状病毒病(COVID-19)相关的死亡和住院病例,但免疫力的减弱以及能够免疫逃逸的变体的出现表明需要新型SARS-CoV-2疫苗。一种鼻内给药的副流感病毒5(PIV5)载体COVID-19疫苗CVXGA1已在动物模型中证明有效,并能阻断雪貂中SARS-CoV-2的接触传播。CVXGA1疫苗目前正在美国进行人体临床试验。这项研究调查了CVXGA1和其他表达额外抗原SARS-CoV-2核蛋白(N)或β、δ、γ和奥密克戎变体的SARS-CoV-2变体刺突(S)蛋白的PIV5载体疫苗在仓鼠中针对同源和异源攻击的免疫原性和效力。单剂量鼻内接种CVXGA1可诱导针对SARS-CoV-2 WA1(原始毒株)、δ变体和奥密克戎变体的中和抗体,并能抵御同源和异源病毒攻击。与mRNA COVID-19疫苗相比,CVXGA1诱导的中和抗体滴度随时间保持良好。当在两剂mRNA COVID-19疫苗后作为加强针给药时,表达来自WA1(CVXGA1)、δ或奥密克戎变体的S蛋白的PIV5载体疫苗与三剂mRNA疫苗相比,能产生更高水平的交叉反应中和抗体。除了S蛋白外,通过攻击感染后最高体重增加评估,N蛋白还提供了额外的保护。我们的数据表明,PIV5载体COVID-19疫苗,如CVXGA1,可作为针对新出现变体的加强针疫苗。
