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携带人呼吸道合胞病毒融合糖蛋白基因的鼠肺炎病毒在恒河猴中高度减毒和免疫原性。

Murine Pneumonia Virus Expressing the Fusion Glycoprotein of Human Respiratory Syncytial Virus from an Added Gene Is Highly Attenuated and Immunogenic in Rhesus Macaques.

机构信息

RNA Viruses Section, Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland, USA.

Institut für Mikrobiologie, Technische Universität Braunschweig, Braunschweig, Germany.

出版信息

J Virol. 2018 Aug 16;92(17). doi: 10.1128/JVI.00723-18. Print 2018 Sep 1.

Abstract

Human respiratory syncytial virus (RSV) continues to be the leading viral cause of severe acute lower respiratory tract disease in infants and children worldwide. A licensed vaccine or antiviral drug suitable for routine use remains unavailable. Like RSV, (MPV) is a member of the genus , family Humans are not normally exposed to MPV, and MPV is not cross-protective with RSV. We evaluated MPV as an RSV vaccine vector expressing the RSV fusion (F) glycoprotein. The RSV F open reading frame (ORF) was codon optimized, and the encoded RSV F protein was made identical to an early passage of RSV strain A2. The RSV F ORF was placed under the control of MPV transcription signals and inserted at the first (rMPV-F1), third (rMPV-F3), or fourth (rMPV-F4) gene position of a version of the MPV genome that contained a codon-pair-optimized polymerase (L) gene. The recovered viruses replicated as efficiently as the empty vector, with stable expression of RSV F protein. Replication and immunogenicity of rMPV-F1 and rMPV-F3 were evaluated in rhesus macaques following intranasal and intratracheal administration. Both viruses replicated at low levels in the upper and lower respiratory tracts, maintained stable RSV F expression, and induced RSV-neutralizing serum antibodies at high levels similar to those induced by wild-type RSV replicating to a 5- to 25-fold-higher titer. In conclusion, this study demonstrated that rMPV provides a highly attenuated yet immunogenic vector for the expression of RSV F protein, with potential application in RSV-naive and RSV-experienced populations. Human respiratory syncytial virus (RSV) is an important human pathogen that lacks a licensed vaccine or antiviral drug suitable for routine use. We describe here the evaluation of recombinant murine pneumonia virus (rMPV) as a live-attenuated vector that expresses the RSV F protein, the major RSV neutralization antigen, as an experimental RSV vaccine. The rMPV-RSV-F vectors expressing RSV F from the first, third, or fourth gene position were genetically stable and were not restricted for replication In contrast, the vectors exhibited highly attenuated replication in the respiratory tract of rhesus macaques, maintained stable RSV F expression, and induced RSV-neutralizing serum antibodies at high titers similar to those conferred by wild-type RSV. Given the lack of preexisting immunity to MPV in humans and the lack of cross-neutralization and cross-protection between MPV and RSV, an rMPV-vectored RSV vaccine should be immunogenic in both RSV-naive children and RSV-experienced adults.

摘要

人类呼吸道合胞病毒(RSV)仍然是全球婴儿和儿童严重急性下呼吸道疾病的主要病毒病因。目前尚无适合常规使用的授权疫苗或抗病毒药物。与 RSV 类似,(MPV)是副黏液病毒科的一个属,人类通常不会接触到 MPV,MPV 也不能与 RSV 交叉保护。我们评估了作为 RSV 融合(F)糖蛋白表达载体的 MPV。RSV F 开放阅读框(ORF)经过密码子优化,编码的 RSV F 蛋白与 RSV 株 A2 的早期传代相同。RSV F ORF 置于 MPV 转录信号的控制下,并插入 MPV 基因组的第一个(rMPV-F1)、第三个(rMPV-F3)或第四个(rMPV-F4)基因位置,该基因组包含一个密码子对优化的聚合酶(L)基因。回收的病毒与空载体一样有效地复制,稳定表达 RSV F 蛋白。在恒河猴中通过鼻腔内和气管内给药评估了 rMPV-F1 和 rMPV-F3 的复制和免疫原性。两种病毒在上呼吸道和下呼吸道均低水平复制,稳定表达 RSV F 表达,并诱导 RSV 中和血清抗体水平与野生型 RSV 复制到 5 至 25 倍更高滴度相似。总之,本研究表明 rMPV 为 RSV F 蛋白表达提供了一种高度减毒但具有免疫原性的载体,具有在 RSV 初免和 RSV 经验人群中的应用潜力。人类呼吸道合胞病毒(RSV)是一种重要的人类病原体,目前尚无适合常规使用的授权疫苗或抗病毒药物。我们在此描述了重组鼠肺炎病毒(rMPV)作为一种活减毒载体的评估,该载体表达 RSV F 蛋白,这是 RSV 的主要中和抗原,作为实验性 RSV 疫苗。表达 RSV F 的 rMPV-RSV-F 载体从第一个、第三个或第四个基因位置表达,遗传稳定,不受限制。相反,载体在恒河猴的呼吸道中表现出高度减毒复制,稳定表达 RSV F,并诱导 RSV 中和血清抗体滴度与野生型 RSV 相似。鉴于人类对 MPV 缺乏预先存在的免疫力,以及 MPV 和 RSV 之间缺乏中和和交叉保护,rMPV 载体 RSV 疫苗应该在 RSV 初免儿童和 RSV 经验成人中均具有免疫原性。

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