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采用支链赖氨酸寡肽法研制的用于人类免疫缺陷病毒感染的多组分肽疫苗具有强大的免疫原性。

Strong immunogenicity of a multicomponent peptide vaccine developed with the branched lysine oligopeptide method for human immunodeficiency virus infection.

作者信息

Okuda K, Kaneko T, Yamakawa T, Tanaka S, Shigematsu T, Yamamoto A, Hamajima K, Nakajima K, Kawamoto S, Phanuphak P

机构信息

Department of Bacteriology, Yokohama City University School of Medicine, Fukuura, Japan.

出版信息

J Mol Recognit. 1993 Sep;6(3):101-9. doi: 10.1002/jmr.300060302.

Abstract

We synthesized one V3 peptide each from HTLV-IIIB, Thai A and Thai B, conjugating them to the T cell epitope of the env region, and we also synthesized a p17 protein peptide of the gag region (HGP-30). These peptides were then coupled to 8-lysine copolymers using N-succinimidyl maleimido carboxylate (M(r) = ca 60,000). We designated this the branched lysine oligopeptide method. The large peptide complexes constructed from these four macromolecular peptides were used with aluminium hydroxide or complete Freund's adjuvant to immunize mice and rabbits four times. ELISA assay showed high titres of anti-peptide antibodies to each V3 loop peptide and the HGP-30 peptide. Strong inhibition of CD4+ dependent cell fusion was obtained with these antisera when IIIB, Thai A and Thai B strains of the human immunodeficiency virus (HIV) were used. Strong anti-fusion inhibition was also observed with two other HIV strains. In addition, an increase of the anti-HIV effect was observed when we used sera obtained by multicomponent vaccine immunization. The same kind of inhibition was also observed in p24 assay systems using these immunized antisera. Activation of IL-2 production in lymphocytes was observed in mice immunized with this vaccine. These results suggest that immunization with macromolecular peptide complexes can result in strong immunogenicity towards HIV-1.

摘要

我们从HTLV-IIIB、泰国A株和泰国B株中各合成了一种V3肽,并将它们与env区域的T细胞表位偶联,我们还合成了gag区域的p17蛋白肽(HGP-30)。然后使用N-琥珀酰亚胺马来酰亚胺羧酸盐(分子量约为60,000)将这些肽与8-赖氨酸共聚物偶联。我们将此命名为分支赖氨酸寡肽法。由这四种大分子肽构建的大肽复合物与氢氧化铝或完全弗氏佐剂一起用于对小鼠和兔子进行四次免疫。ELISA检测显示针对每种V3环肽和HGP-30肽的抗肽抗体具有高滴度。当使用人类免疫缺陷病毒(HIV)的IIIB、泰国A株和泰国B株时,这些抗血清对CD4 +依赖性细胞融合有强烈抑制作用。对另外两种HIV毒株也观察到了强烈的抗融合抑制作用。此外,当我们使用多组分疫苗免疫获得的血清时,观察到抗HIV效果增强。在使用这些免疫抗血清的p24检测系统中也观察到了同样的抑制作用。在用这种疫苗免疫的小鼠中观察到淋巴细胞中IL-2产生的激活。这些结果表明,用大分子肽复合物免疫可对HIV-1产生强烈的免疫原性。

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