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Overcoming Immunity to a Viral Vaccine by DNA Priming before Vector Boosting

机译:在载体加强前通过DNA引物克服病毒疫苗的免疫力

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摘要

Replication-defective adenovirus (ADV) and poxvirus vectors have shown potential as vaccines for pathogens such as Ebola or human immunodeficiency virus in nonhuman primates, but prior immunity to the viral vector in humans may limit their clinical efficacy. To overcome this limitation, the effect of prior viral exposure on immune responses to Ebola virus glycoprotein (GP), shown previously to protect against lethal hemorrhagic fever in animals, was studied. Prior exposure to ADV substantially reduced the cellular and humoral immune responses to GP expressed by ADV, while exposure to vaccinia inhibited vaccine-induced cellular but not humoral responses to GP expressed by vaccinia. This inhibition was largely overcome by priming with a DNA expression vector before boosting with the viral vector. Though heterologous viral vectors for priming and boosting can also overcome this effect, the paucity of such clinical viral vectors may limit their use. In summary, it is possible to counteract prior viral immunity by priming with a nonviral, DNA vaccine.
机译:复制缺陷型腺病毒(ADV)和痘病毒载体已显示出在非人类灵长类动物中作为病原体(如埃博拉病毒或人类免疫缺陷病毒)的疫苗的潜力,但对人类病毒载体的先前免疫可能会限制其临床疗效。为了克服这一局限性,研究了先前病毒暴露对埃博拉病毒糖蛋白(GP)免疫反应的影响,该作用先前已证明可防止动物的致命性出血热。事先暴露于ADV会大大降低ADV表达的对GP的细胞和体液免疫反应,而暴露于牛痘会抑制疫苗诱导的对痘苗所表达的GP的细胞反应但不是体液。通过在用病毒载体加强免疫之前用DNA表达载体引发,可以大大克服这种抑制作用。尽管用于引发和加强的异源病毒载体也可以克服这种作用,但是这种临床病毒载体的缺乏可能会限制其使用。总之,可以通过用非病毒的DNA疫苗进行免疫来抵消先前的病毒免疫。

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