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对共价连接于脂质体表面和包封于脂质体内的脊髓灰质炎肽的免疫反应比较。

Comparison of the immune response against polio peptides covalently-surface-linked to and internally-entrapped in liposomes.

作者信息

Tan L, Weissig V, Gregoriadis G

机构信息

Department of Pharmacology, Faculty of Medicine, National University of Singapore, Kent Ridge.

出版信息

Asian Pac J Allergy Immunol. 1991 Jun;9(1):25-30.

PMID:1663745
Abstract

The adjuvanticity of liposomes on two different modes of presentation of polio virus subunit peptides was demonstrated by incorporating the poorly immunogenic synthetic polio peptides, W1 and W2, into the internal space of and covalently-linked to the surface of dehydration-rehydration vesicles (DRV). It was found that for both peptides, liposome association in either mode boosted the primary and secondary IgG1 responses against 5 micrograms peptide as compared to controls in which free peptide was administered. Surface-linkage of peptides (both W1 and W2) exhibited an initially more rapid rise in antibody levels, as compared to internal entrapment of the peptides, but elicited no observable secondary response. However, although encapsulated W1 showed a milder primary response when compared to the surface-linked formulation, it later elicited a strong secondary response. These results suggested that it may be advantageous to administer liposomal virus subunit vaccines in both surface-linked and internally entrapped formulations to achieve adequate initial antibody levels followed by an anamnestic response.

摘要

通过将免疫原性较差的合成脊髓灰质炎肽W1和W2分别包封于脱水-再水化囊泡(DRV)内部空间以及共价连接到其表面,证实了脂质体对脊髓灰质炎病毒亚基肽两种不同呈递方式的佐剂效应。结果发现,与注射游离肽的对照组相比,两种肽以任何一种方式与脂质体结合,均可增强针对5微克肽的初次和二次IgG1应答。与肽包封于内部相比,肽(W1和W2)与表面连接时抗体水平最初上升更快,但未引发可观察到的二次应答。然而,尽管与表面连接制剂相比,包封的W1初次应答较弱,但随后引发了强烈的二次应答。这些结果表明,同时使用表面连接和内部包封制剂来接种脂质体病毒亚基疫苗,可能有利于在获得足够初始抗体水平的同时引发回忆应答。

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