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A bivalent HCV peptide vaccine elicits pan-genotypic neutralizing antibodies in mice

机译:一只二价HCV肽疫苗引发小鼠的泛基因型中和抗体

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Vaccine development for antigenically variable pathogens has faltered because extreme genetic diversity precludes induction of broadly neutralizing antibodies (nAB) with classical vaccines. Here, using the most variable epitope of any known human pathogen (HVR1 of HCV), we describe a novel approach capable of eliciting broadly neutralizing antibodies targeting highly variable epitopes. Our proof-of-concept vaccine elicited pan-genotypic nAB against HCV variants differing from the immunogen sequences by more than 70% at the amino acid level. These findings suggest broadly nAB to highly variable pathogens can be elicited by vaccines designed to target physicochemically conserved residues within hypervariable epitopes. (c) 2020 Elsevier Ltd. All rights reserved.
机译:抗原性可变病原体的疫苗开发致力于,因为极端遗传多样性妨碍诱导近似中和抗体(NAB)与经典疫苗。 这里,使用任何已知人类病原体(HCV的HVR1)的最可变的表位,我们描述了一种能够引发靶向高度可变表位的宽度中和抗体的新方法。 我们的概念证据疫苗引发了泛基因型Nab对氨基酸水平在70%以上与免疫原序列不同的HCV变体。 这些研究结果表明,广泛的可变病原体可以通过旨在靶向靶向靶向高变性表位内的物理化学保守残留物的疫苗引发。 (c)2020 elestvier有限公司保留所有权利。

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