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首页> 外文期刊>Clinical and diagnostic laboratory immunology >Poliovirus-specific immunoglobulin A in persons vaccinated with inactivated poliovirus vaccine in The Netherlands.
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Poliovirus-specific immunoglobulin A in persons vaccinated with inactivated poliovirus vaccine in The Netherlands.

机译:在荷兰接种灭活的脊髓灰质炎疫苗的人群中有脊灰病毒特异性免疫球蛋白A。

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In The Netherlands the inactivated poliovirus vaccine (IPV) is used for protection against poliomyelitis. It is not clear if parenteral vaccination with IPV can lead to priming of the mucosal immune system. We developed and evaluated enzyme-linked immunosorbent assays for the detection of poliovirus serotype-specific immunoglobulin A (IgA) and secretory IgA antibodies. Using these assays we examined the kinetics of the IgA response in sequential serum samples from 15 poliomyelitis patients after natural infection with serotype 3 poliovirus. In 36% of the patients IgA remained present for up to 5 months postinfection. Furthermore, we examined, in an IPV-vaccinated population, the presence of IgA antibodies in sera from young children (4 to 12 years of age; n = 177), sera from older children (between 13 and 15 years of age; n = 123), sera from healthy blood donors (n = 66), and sera from naturally immune elderly persons (n = 54). The seroprevalence of IgA to all three serotypes was low in young vaccinated children (5 to 7%), and the seroprevalence of IgA types 2 and 3 was low in older vaccinated children (2 to 3%). The seroprevalence of antibodies to type 1 was significantly higher (18%) in older children than in younger children. This higher seroprevalence is most likely explained by the persistence of IgA following infection with the serotype 1 wild-type poliovirus strain during the 1978 epidemic. In healthy adults, the seroprevalence of type 1- and type 2-specific IgA was significantly higher than that in young children. These results suggest that at least part of the IgA found in the older population is induced by infections unrelated to the IPV vaccination schedule. Finally, we found that parenteral vaccination with IPV was able to boost secretory IgA responses in 74 to 87% of a naturally exposed elderly population (n = 54). While the presence of secretory IgA in IPV-vaccinated persons has been documented previously, our findings suggest that mucosal priming with live virus is necessary to obtain an IgA response after IPV booster vaccination.
机译:在荷兰,灭活的脊髓灰质炎病毒疫苗(IPV)用于预防脊髓灰质炎。肠胃外接种IPV疫苗是否可以引发粘膜免疫系统尚不清楚。我们开发并评估了用于检测脊髓灰质炎病毒血清型特异性免疫球蛋白A(IgA)和分泌型IgA抗体的酶联免疫吸附法。使用这些试验,我们检查了血清型3脊髓灰质炎病毒自然感染后,来自15名脊髓灰质炎患者的连续血清样本中IgA反应的动力学。在感染后长达5个月的患者中,有36%的患者存在IgA。此外,我们在接受IPV疫苗接种的人群中检查了年幼儿童(4至12岁; n = 177),大龄儿童(13至15岁; n = 123),健康献血者的血清(n = 66)和自然免疫老年人的血清(n = 54)。在年轻的接种儿童中,IgA对所有三种血清型的血清阳性率均较低(5%至7%),在年龄较大的接种儿童中,IgA 2型和3型的血清阳性率较低。与年龄较小的儿童相比,年龄较大的儿童的1型抗体的血清阳性率明显更高(18%)。 1978年流行期间,血清1型野生型脊髓灰质炎病毒株感染后IgA持续存在,很可能解释了这种较高的血清阳性率。在健康的成年人中,1型和2型特异性IgA的血清阳性率显着高于幼儿。这些结果表明,在老年人群中发现的至少部分IgA是由与IPV疫苗接种时间表无关的感染诱导的。最后,我们发现IPV的肠胃外疫苗接种能够提高74%至87%的自然暴露的老年人口(n = 54)的分泌型IgA反应。虽然以前已记录了IPV疫苗接种者中分泌型IgA的存在,但我们的发现表明,在IPV加强疫苗接种后,用活病毒进行粘膜引发对于获得IgA反应是必要的。

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