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多克隆抗独特型抗体诱导抗血凝素抗体的产生。

Induction of antihemagglutinin antibodies by polyclonal antiidiotype antibodies.

作者信息

Dinca L, Neuwirth S, Schulman J, Bona C

机构信息

Department of Microbiology, Mount Sinai School of Medicine, New York, New York.

出版信息

Viral Immunol. 1993 Spring;6(1):75-84. doi: 10.1089/vim.1993.6.75.

Abstract

Antiidiotypic antibodies can be envisioned as an alternative approach in the development of vaccines against influenza virus, which exhibits natural antigenic variations. In our work, we obtained two polyclonal cross-reactive anti-Id antibodies against PY102, VM113, and VM202 mAbs, which in turn are specific respectively for PR8 virus and laboratory-induced virus variants (PY102-V1 and VM113-V1). With these cross-reactive anti-Id antibodies, we were able to elicit anti-HA antibodies in mice. In comparing the anti-HA antibody response in animals injected with anti-Id antibodies to those immunized with PR8 influenza virus, we demonstrated that the HI titer was higher after virus immunization and that the PR8 virus boost was more efficient in this group. Our results showed that the polyclonal cross-reactive anti-Id antibodies were more efficient than the individual anti-Ids at eliciting responses. At the same time, we demonstrated that PR8-primed T cells, cultured with B cells from animals immunized with anti-Id antibodies, were able to produce anti-PR8 antibodies subsequent to stimulation with influenza virus.

摘要

抗独特型抗体可被视为开发针对流感病毒疫苗的一种替代方法,流感病毒具有天然的抗原变异。在我们的研究中,我们获得了两种针对PY102、VM113和VM202单克隆抗体的多克隆交叉反应抗独特型抗体,而这些单克隆抗体又分别对PR8病毒和实验室诱导的病毒变体(PY102-V1和VM113-V1)具有特异性。利用这些交叉反应抗独特型抗体,我们能够在小鼠体内诱导产生抗血凝素(HA)抗体。在比较注射抗独特型抗体的动物与接种PR8流感病毒的动物的抗HA抗体反应时,我们发现病毒免疫后血凝抑制(HI)效价更高,并且该组中PR8病毒加强免疫更有效。我们的结果表明,多克隆交叉反应抗独特型抗体在引发反应方面比单个抗独特型抗体更有效。同时,我们证明,用来自接种抗独特型抗体动物的B细胞培养的经PR8致敏的T细胞,在受到流感病毒刺激后能够产生抗PR8抗体。

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