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In vivo evolution of the gp90 gene and consistently low plasma viral load during transient immune suppression demonstrate the safety of an attenuated equine infectious anemia virus (EIAV) vaccine

机译:gp90基因的体内进化以及瞬时免疫抑制过程中血浆病毒载量始终较低,证明了减毒马传染性贫血病毒(EIAV)疫苗的安全性

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摘要

To study the in vivo evolution of the attenuated Chinese equine infectious anemia virus (EIAV) vaccine, viral gp90 gene variation and virus replication in immunosuppressed hosts were investigated. The results showed that after vaccination, the gp90 gene followed an evolutionary trend of declining diversity. The trend coincided with the maturation of immunity to EIAV, and eventually, the gp90 gene became highly homologous. The sequences of these predominant quasispecies were consistently detected up to 18 months after vaccination. Furthermore, after transient immune suppression with dexamethasone, the plasma viral RNA copy number of the vaccine strain in three vaccinated ponies remained consistently below the “pathogenic threshold” level, while the viral load increased by 25,000-fold in the positive control of an inapparent carrier of the parental virulent strain. This study is the first to provide evidence for the safety of an attenuated lentiviral vaccine with decreased genomic diversity and consistently low viral replication under suppressed immunity.
机译:为了研究减毒的中国马传染性贫血病毒(EIAV)疫苗的体内进化,研究了免疫抑制宿主中的病毒gp90基因变异和病毒复制。结果表明,接种疫苗后,gp90基因遵循多样性下降的进化趋势。这种趋势与针对EIAV的免疫力的成熟相吻合,最终,gp90基因变得高度同源。这些主要的准种的序列在接种疫苗后的18个月内一直被检测到。此外,在使用地塞米松进行短暂免疫抑制后,在三个接种小马中疫苗株的血浆病毒RNA拷贝数始终保持低于“致病性阈值”水平,而在无明显载体的阳性对照中,病毒载量增加了25,000倍。父母毒株。这项研究是第一个为减毒慢病毒疫苗的安全性提供证据的方法,该疫苗具有降低的基因组多样性和在抑制免疫力的情况下持续低水平的病毒复制。

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