Induction of antibodies against the Plasmodium falciparum p126 antigen in non-responder H-2b and partial-responder H-2d mice using synthetic peptides.

Peptide research Pub Date : 1996-03-01
M Gilardeau Truffinet, M Bossus, D Camus, P Delplace, C Mazingue, E Diesis, A Tartar, S Moreau, H Gras-Masse, D M Banic
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Abstract

The p126 Plasmodium falciparum antigen is processed into two fragments, p50 and p73, the latter one containing the subfragments p47 and p18 when the schizonts rupture. An absence of antibody response against the p126 antigen has been reported recently in H-2b mice and limited to the p73 processed fragment in H-2d mice. Synthetic peptides corresponding to various domains of the molecule have been used to immunize mice in order to overcome the absence of an immune response. Synthetic peptides corresponding to the N-terminus of p50 or p18 as well as to the C-terminus of p47 were unable to induce anti-peptide antibodies when injected carrier-free or coupled to ovalbumin. Synthetic peptides corresponding to the C-terminus of p18 or composed of 6 or 9 serines were able to induce anti-peptide antibodies when injected coupled to a carrier protein. However, none of these antibodies was able to recognize the native p126 molecule. Various synthetic peptides corresponding to the 6-octapeptide [Nt47 (6 x 8)] or the 4-octapeptide [Nt47(4 x 8)] repeat sequence localized at the N-terminus of the p47 have also been used to immunize mice. No antibodies were generated using a carrier-free [Nt47(6 x 8)-Cys]2 or [Nt47 (4 x 8)-Cys]2 peptide, an octameric multiple antigen peptide construct [Nt47(6 x 8)]-MAP or the [Nt47(6 x 8)] coupled to one or two palmitic acids. In contrast, [Nt47(6 x 8)]-Cys coupled to either tetanus toxoid (TT) or ovalbumin (OVA) and [Nt47(4 x 8)]-Cys coupled to OVA induced antibodies against the synthetic peptide and the native p126 molecule in both H-2d and H-2b mice. A multiple antigen peptide construct [Nt47(4 x 8)-MSP-3b]-MAP containing 4 [Nt47(4 x 8)] and 4 [MSP-3b] also induced antibodies against the synthetic peptide [Nt47(4 x 8)-Cys]2 and the native p126 molecule in both H-2d and H-2b mice.

利用合成肽诱导无应答H-2b和部分应答H-2d小鼠抗恶性疟原虫p126抗原抗体。
p126恶性疟原虫抗原被加工成p50和p73两个片段,当分裂体破裂时,后者含有p47和p18亚片段。最近有报道称在H-2b小鼠中缺乏针对p126抗原的抗体反应,而在H-2d小鼠中仅限于p73加工片段。合成肽对应的分子的各种领域已被用于免疫小鼠,以克服缺乏免疫反应。人工合成的p50或p18的n端和p47的c端对应的肽在无载体注射或与卵清蛋白偶联时不能诱导抗肽抗体。与p18的c端对应或由6或9个丝氨酸组成的合成肽与载体蛋白偶联注射时能够诱导抗肽抗体。然而,这些抗体都不能识别天然的p126分子。各种合成肽对应于6-八肽[Nt47(6 × 8)]或4-八肽[Nt47(4 × 8)]重复序列定位在p47的n端也被用于免疫小鼠。使用无载体的[Nt47(6 × 8)-Cys]2或[Nt47(4 × 8)-Cys]2肽,与一种或两种棕榈酸偶联的八聚体多抗原肽结构[Nt47(6 × 8)]-MAP或[Nt47(6 × 8)]不产生抗体。相反,在H-2d和H-2b小鼠中,[Nt47(6 × 8)]-Cys与破伤风类毒素(TT)或卵清蛋白(OVA)偶联,[Nt47(4 × 8)]-Cys与OVA偶联诱导了针对合成肽和天然p126分子的抗体。含有4 [Nt47(4 × 8)]和4 [MSP-3b]的多抗原肽构建物[Nt47(4 × 8)-MSP-3b]-MAP也在H-2d和H-2b小鼠中诱导了针对合成肽[Nt47(4 × 8)-Cys]2和天然p126分子的抗体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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