Solid phase synthesis and immunogenicity of a VP3 peptide from hepatitis A virus.

J A Pérez, J F González-Dankaart, F Reig, R M Pintó, A Bosch, I Haro
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Abstract

The synthesis of a peptide belonging to the VP3 capsid protein of Hepatitis A virus has been accomplished by the continuous flow Fmoc-polyamide solid phase method. The use of methoxytrimethylbenzenesulphonyl (Mtr) and pentamethylchromansulphonyl (Pmc) as arginine side-chain protecting groups in the presence of tryptophan without lateral protection or protected with t-Boc is discussed. The synthetic VP3 peptide has been administered to mice in different forms: (i) free, (ii) coupled to keyhole limpet hemocyanin, (iii) encapsulated in multilamellar (MLV) liposomes, and (iv) incorporated to a tetrameric branched lysine core. The immune response induced by these preparation is reported.

甲型肝炎病毒VP3肽的固相合成及其免疫原性。
采用连续流动fmoc -聚酰胺固相法合成了甲型肝炎病毒VP3衣壳蛋白的肽段。讨论了在色氨酸存在下,甲氧基三甲基苯磺酰基(Mtr)和五甲基氯磺酰基(Pmc)作为精氨酸侧链保护基团的使用。合成的VP3肽以不同的形式给药于小鼠:(i)游离,(ii)与锁孔帽贝血青素偶联,(iii)封装在多层(MLV)脂体中,(iv)与四聚体支链赖氨酸核心结合。报道了这些制剂引起的免疫反应。
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