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A Plant-Produced in vivo deglycosylated full-length Pfs48/45 as a Transmission-Blocking Vaccine Candidate against malaria

机译:植物生产的体内去糖基化全长Pfs48 / 45作为抗疟疾的传播阻断疫苗候选者

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摘要

Pfs48/45 is a leading antigen candidate for a transmission blocking (TB) vaccine. However, efforts to produce affordable, safe and correctly folded full-length Pfs48/45 using different protein expression systems have not produced an antigen with satisfactory TB activity. Pfs48/45 has 16 cysteines involved in disulfide bond formation, and the correct formation is critical for proper folding and induction of TB antibodies. Moreover, Pfs48⁄45 is not a glycoprotein in the native hosts, but contains potential glycosylation sites, which are aberrantly glycosylated during expression in eukaryotic systems. Here, we demonstrate for the first time that full length, Endo H in vivo enzymatic deglycosylated Pfs48/45 antigen is produced at a high level in plants and is structurally stable at elevated temperatures. Sera from mice immunized with this antigen showed strong inhibition in SMFA. Thus, Endo H in vivo enzymatic deglycosylated Pfs48/45 is a promising candidate for the development of an affordable TB vaccine, which may have the potential to save millions.
机译:Pfs48 / 45是传播阻断(TB)疫苗的领先抗原候选物。但是,使用不同的蛋白质表达系统生产价格合理,安全且正确折叠的全长Pfs48 / 45的努力并未产生具有令人满意的TB活性的抗原。 Pfs48 / 45具有16个半胱氨酸参与二硫键的形成,正确的形成对于正确折叠和诱导TB抗体至关重要。此外,Pfs48⁄45在天然宿主中不是糖蛋白,但包含潜在的糖基化位点,这些位点在真核系统中表达过程中被异常糖基化。在这里,我们首次证明了全长的Endo H体内酶促去糖基化Pfs48 / 45抗原在植物中高水平产生,并且在高温下结构稳定。用这种抗原免疫的小鼠的血清在SMFA中显示出强烈的抑制作用。因此,Endo H体内酶促去糖基化的Pfs48 / 45是开发负担得起的TB疫苗的有希望的候选者,它可能具有节省数百万美元的潜力。

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