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Live attenuated influenza vaccine provides superior protection from heterologous infection in pigs with maternal antibodies without inducing vaccine associated enhanced respiratory disease

机译:减毒活流感疫苗可提供卓越的保护,使其免受母源抗体感染的猪的异源感染,而不会引起疫苗相关的增强呼吸道疾病

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摘要

Control of swine influenza A virus (IAV) in the US is hindered since inactivated vaccines do not provide robust cross‐protection against the multiple antigenic variants co‐circulating in the field. Vaccine efficacy can be further limited when administered to young pigs that possess maternally derived immunity. We previously demonstrated a recombinant A/sw/Texas/4199‐2/1998 (TX98) (H3N2) expressing a truncated NS1 protein is attenuated in swine and has potential for use as an intranasal live attenuated influenza virus (LAIV) vaccine. In the present study, we compared 1 dose of intranasal LAIV with 2 intramuscular doses of TX98 whole inactivated virus (WIV) with adjuvant in weanling pigs with and without TX98‐specific maternally‐derived antibodies (MDA). Pigs were subsequently challenged with wild type homologous TX98 H3N2 virus or with an antigenic variant A/sw/Colorado/23619/1999 (CO99) (H3N2). In the absence of MDA, both vaccines protected against homologous TX98 and heterologous CO99 shedding, although the LAIV elicited lower hemagglutination inhibiting (HI) antibody titers in serum. The efficacy of both vaccines was reduced by the presence of MDA; however, WIV vaccination of MDA‐positive pigs led to dramatically enhanced pneumonia following heterologous challenge, a phenomenon known as vaccine‐associated enhanced respiratory disease (VAERD). A single‐dose of LAIV to MDA‐positive pigs still provided partial protection from CO99 and may be a safer vaccine for young pigs in field conditions where dams are routinely vaccinated and diverse IAV strains are in circulation. These results have implications not only to pigs but to other influenza virus host species.
机译:由于灭活疫苗无法针对现场共同流行的多种抗原变体提供强大的交叉保护作用,因此阻碍了美国对A型猪流感病毒(IAV)的控制。当对具有母源性免疫力的幼猪给药时,疫苗效力可能会进一步受到限制。我们先前证明了重组A / sw / Texas / 4199-2-2 / 1998(TX98)(H3N2)表达的NS1截短蛋白在猪中减毒,并且有潜力用作鼻内减毒流感病毒(LAIV)疫苗。在本研究中,我们比较了在有和没有TX98特异性母源抗体(MDA)的断奶猪中,将1剂鼻内LAIV与2肌内剂量TX98全灭活病毒(WIV)与佐剂进行比较。随后用野生型同源TX98 H3N2病毒或抗原变体A / sw / Colorado / 23619/1999(CO99)(H3N2)攻击猪。在没有MDA的情况下,尽管LAIV引起血清中较低的血凝抑制(HI)抗体效价,但两种疫苗均能防止同源TX98和异源CO99脱落。 MDA的存在降低了两种疫苗的效力;但是,MDA阳性猪的WIV疫苗接种导致异源性感染后肺炎急剧增加,这种现象被称为疫苗相关性增强呼吸道疾病(VAERD)。单剂LAIV到MDA阳性猪仍可部分保护CO99,对于在常规大坝常规疫苗接种和多种IAV株流通的野外条件下的幼猪来说,这可能是一种更安全的疫苗。这些结果不仅对猪有影响,而且对其他流感病毒宿主也有影响。

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