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人类和非人类灵长类动物在初次感染或再次感染3型副流感病毒后,针对血凝素神经氨酸酶和融合糖蛋白的各个抗原位点的抗体反应。

Antibody responses of humans and nonhuman primates to individual antigenic sites of the hemagglutinin-neuraminidase and fusion glycoproteins after primary infection or reinfection with parainfluenza type 3 virus.

作者信息

van Wyke Coelingh K L, Winter C C, Tierney E L, Hall S L, London W T, Kim H W, Chanock R M, Murphy B R

机构信息

Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, Maryland 20892.

出版信息

J Virol. 1990 Aug;64(8):3833-43. doi: 10.1128/JVI.64.8.3833-3843.1990.

Abstract

An unusual feature of human parainfluenza virus type 3 (PIV3) is ita ability to cause reinfection with high efficiency. The antibody responses of 45 humans and 9 rhesus monkeys to primary infection or subsequent reinfection with PIV3 were examined to identify deficiencies in host immunologic responses that might contribute to the ability of the virus to cause reinfection with high frequency. Antibody responses in serum were tested by using neutralization and hemagglutination inhibition (HI) assays and a monoclonal antibody blocking immunoassay able to detect antibodies to epitopes within six antigenic sites on the PIV3 hemagglutinin-neuraminidase (HN) glycoprotein and eight antigenic sites on the fusion (F) protein. Primary infection of seronegative infants or children with PIV3 stimulated strong and rather uniform HI and neutralizing antibody responses. More than 90% of the individuals developed antibodies to four of the six HN antigenic sites (including three of the four neutralization sites), but the responses to F antigenic sites were of lesser magnitude and varied considerably from person to person. Young infants who possessed maternally derived antibodies in their sera developed lower levels and less frequent HI, neutralizing, and antigenic site-specific responses to the HN and F glycoproteins than did seronegative infants and children. In contrast, children reinfected with PIV3 developed even higher HI and neutralizing antibody responses than those observed during primary infection. Reinfection broadened the HN and F antigenic site-specific responses, but the latter remained relatively restricted. Adults possessed lower levels of HI, neutralizing, and antigenic site-specific antibodies in their sera than did children who had been reinfected, suggesting that these antibodies decay with time. Rhesus monkeys developed more vigorous primary and secondary antibody responses than did humans, but even in these highly responsive animals, response to the F glycoprotein was relatively restricted following primary infection. Bovine PIV3 induced a broader response to human PIV3 in monkeys than was anticipated on the basis of their known relatedness as defined by using monoclonal antibodies to human PIV3. These observations suggest that the restricted antibody responses to multiple antigenic sites on the F glycoprotein in young seronegative infants and children and the decreased responses to both the F and HN glycoproteins in young infants and children with maternally derived antibodies may play a role in the susceptibility of human infants and young children to reinfection with PIV3.

摘要

人类3型副流感病毒(PIV3)的一个不寻常特征是其高效引发再次感染的能力。对45名人类和9只恒河猴针对PIV3初次感染或随后再次感染的抗体反应进行了检测,以确定宿主免疫反应中的缺陷,这些缺陷可能导致该病毒高频引发再次感染。通过使用中和试验、血凝抑制(HI)试验以及一种单克隆抗体阻断免疫测定法来检测血清中的抗体反应,该单克隆抗体阻断免疫测定法能够检测针对PIV3血凝素神经氨酸酶(HN)糖蛋白上六个抗原位点以及融合(F)蛋白上八个抗原位点内表位的抗体。血清学阴性的婴儿或儿童初次感染PIV3会刺激产生强烈且相当一致的HI和中和抗体反应。超过90%的个体产生了针对六个HN抗原位点中四个位点(包括四个中和位点中的三个)的抗体,但对F抗原位点的反应程度较低,且个体之间差异很大。血清中含有母体来源抗体的幼儿对HN和F糖蛋白产生的HI、中和及抗原位点特异性反应水平较低且频率较低,低于血清学阴性的婴儿和儿童。相比之下,再次感染PIV3的儿童产生的HI和中和抗体反应甚至高于初次感染时观察到的反应。再次感染拓宽了HN和F抗原位点特异性反应,但对F抗原位点的反应仍相对有限。成年人血清中的HI、中和及抗原位点特异性抗体水平低于再次感染过的儿童,这表明这些抗体随时间衰减。恒河猴产生的初次和二次抗体反应比人类更强烈,但即使在这些反应强烈的动物中,初次感染后对F糖蛋白的反应也相对有限。基于使用针对人类PIV3的单克隆抗体所定义的已知亲缘关系,牛PIV3在猴子中引发的针对人类PIV3的反应比预期的更广泛。这些观察结果表明,血清学阴性的幼儿对F糖蛋白多个抗原位点的有限抗体反应,以及含有母体来源抗体的幼儿对F和HN糖蛋白反应的降低,可能在人类婴幼儿易受PIV3再次感染中发挥作用。

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