Swiss Tropical Institute, Molecular Immunology, CH-4002 Basel, Switzerland.
Malar J. 2009 Dec 30;8:314. doi: 10.1186/1475-2875-8-314.
Clinical profiling of two components for a synthetic peptide-based virosomal malaria vaccine has yielded promising results, encouraging the search for additional components for inclusion in a final multi-valent vaccine formulation. This report describes the immunological characterization of linear and cyclized synthetic peptides comprising amino acids 211-237 of Plasmodium falciparum merozoite surface protein (MSP-3).
These peptides were coupled to phosphatidylethanolamine (PE); the conjugates were intercalated into immunopotentiating reconstituted influenza virosomes (IRIVs) and then used for immunizations in mice to evaluate their capacity to elicit P. falciparum cross-reactive antibodies.
While all MSP-3-derived peptides were able to elicit parasite-binding antibodies, stabilization of turn structures by cyclization had no immune-enhancing effect. Therefore, further pre-clinical profiling was focused on FB-12, a PE conjugate of the linear peptide. Consistent with the immunological results obtained in mice, all FB-12 immunized rabbits tested seroconverted and consistently elicited antibodies that interacted with blood stage parasites. It was observed that a dose of 50 microg was superior to a dose of 10 microg and that influenza pre-existing immunity improved the immunogenicity of FB-12 in rabbits. FB-12 production was successfully up-scaled and the immunogenicity of a vaccine formulation, produced according to the rules of Good Manufacturing Practice (GMP), was tested in mice and rabbits. All animals tested developed parasite-binding antibodies. Comparison of ELISA and IFA titers as well as the characterization of a panel of anti-FB-12 monoclonal antibodies indicated that at least the majority of antibodies specific for the virosomally formulated synthetic peptide were parasite cross-reactive.
These results reconfirm the suitability of IRIVs as a carrier/adjuvant system for the induction of strong humoral immune responses against a wide range of synthetic peptide antigens. The virosomal formulation of the FB-12 peptidomimetic is suitable for use in humans and represents a candidate component for a virosomal multi-valent malaria subunit vaccine.
基于合成肽的病毒体疟疾疫苗的两个成分的临床分析取得了可喜的结果,这鼓励了寻找其他成分以纳入最终的多价疫苗配方。本报告描述了包含恶性疟原虫裂殖表面蛋白(MSP-3)氨基酸 211-237 的线性和环化合成肽的免疫学特征。
这些肽与磷脂酰乙醇胺(PE)偶联;将缀合物插入免疫增强型重组流感病毒体(IRIV)中,然后用于免疫小鼠,以评估它们诱导疟原虫交叉反应性抗体的能力。
虽然所有 MSP-3 衍生肽都能够诱导寄生虫结合抗体,但环化稳定转角结构没有免疫增强作用。因此,进一步的临床前分析集中在 FB-12 上,这是线性肽的 PE 缀合物。与在小鼠中获得的免疫学结果一致,所有 FB-12 免疫的兔子均发生血清转化,并且一致地诱导与血液阶段寄生虫相互作用的抗体。观察到 50μg 剂量优于 10μg 剂量,并且流感预先存在的免疫提高了 FB-12 在兔子中的免疫原性。FB-12 的生产成功地扩大规模,并根据良好生产规范(GMP)的规则测试了疫苗制剂在小鼠和兔子中的免疫原性。所有测试的动物均产生寄生虫结合抗体。ELISA 和 IFA 滴度的比较以及抗 FB-12 单克隆抗体的分析表明,至少大多数针对病毒体配方的合成肽特异性抗体是寄生虫交叉反应的。
这些结果再次证实,IRIV 作为诱导针对广泛合成肽抗原的强烈体液免疫反应的载体/佐剂系统是合适的。FB-12 肽模拟物的病毒体配方适合人类使用,是病毒体多价疟疾亚单位疫苗的候选成分。
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