通过红色同源重组和反选择方法,构建基于囊壳显示策略的针对 HAdV4/HAdV7 的二价候选疫苗

IF 3.5 Q1 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH
Peng Wang , Yunting Shao , Xichun Yang , Wenning Zhang , Jianguang Zhou , Fang Huang , Shuang Liu , Jiping Zheng , Chengjun Wu , Shanhu Li
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引用次数: 0

摘要

人类腺病毒(HAdVs)是主要的呼吸道病原体。具体来说,人类腺病毒 4 型(HAdV4)和人类腺病毒 7 型(HAdV7)以引起发烧和肺炎而闻名,并在人群中造成死亡病例。近年来,HAdV4/HAdV7 已在多个国家引起大规模爆发,导致发病率上升。大多数 HAdV4 和 HAdV7 感染报告发生在北美洲、亚洲、欧洲、非洲、南美洲、大洋洲和中东。大多数死亡病例发生在北美(美国)和亚洲(中国和新加坡)。工程重组腺病毒作为疫苗载体发挥了重要作用。在本研究中,我们构建了重组腺病毒 Ad4ITRmut-Ad7E3,并对其进行了体外和体内评估。我们观察到 Ad4ITRmut-Ad7E3 的复制率低于 RI-67 株,这表明倒位末端重复序列(ITR)的突变削弱了 HAdV4 的复制能力。通过腹腔注射和口服给 BALB/c 小鼠接种二价 Ad4ITRmut-Ad7E3 疫苗株,可激发针对 HAdV4 和 HAdV7 的中和抗体。这一发现不仅为高效构建针对 HAdV4 和 HAdV7 的多价重组腺病毒候选疫苗提供了一种新的方法和技术,而且还能针对其他流行的腺病毒血清型,如来自不同地区的 HAdV3、HAdV11、HAdV14 和 HAdV55。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Construction of a bivalent vaccine candidate against HAdV4/HAdV7 based on capsid-display strategy via Red-homologous recombination and counter-selection methodology

Human adenoviruses (HAdVs) are major respiratory pathogens. Specifically, human adenovirus type 4 (HAdV4) and human adenovirus type 7 (HAdV7) are known for causing fever and pneumonia, with documented cases of fatalities among the population. In recent years, HAdV4/HAdV7 has been implicated in causing substantial outbreaks, leading to increased morbidity in multiple countries. Most HAdV4 and HAdV7 infections have been reported in North America, Asia, Europe, Africa, South America, Oceania, and the Middle East. Most fatalities occurred in North America (the United States) and Asia (China and Singapore). Engineered recombinant adenoviruses have played a crucial role as vaccine vectors. In this study, we constructed a recombinant adenovirus, Ad4ITRmut-Ad7E3, and evaluated it in vitro and in vivo. We observed that the replication rate of Ad4ITRmut-Ad7E3 was lower than that of the RI-67 strain, indicating that the mutation of inverted terminal repeats (ITRs) weakened the replication ability of HAdV4. Immunization of BALB/c mice with the bivalent Ad4ITRmut-Ad7E3 vaccine strain, administered by intraperitoneal injection and oral gavage, resulted in the elicitation of neutralizing antibodies targeting HAdV4 and HAdV7. This finding not only provides a novel method and technique for the efficient construction of a polyvalent recombinant adenovirus vaccine candidate against HAdV4 and HAdV7 but also against other prevalent adenovirus serotypes such as HAdV3, HAdV11, HAdV14, and HAdV55, from various regions.

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来源期刊
Biosafety and Health
Biosafety and Health Medicine-Infectious Diseases
CiteScore
7.60
自引率
0.00%
发文量
116
审稿时长
66 days
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