Humoral immune response against proteophosphoglycan surface antigens ofEntamoeba histolyticaelicited by immunization with synthetic mimotope peptides

溶组织内阿米巴 锁孔血蓝蛋白 生物 模拟电影 表位 抗原 噬菌体展示 单克隆抗体 抗体 免疫 免疫系统 微生物学 抗体效价 阿米巴病 病毒学 效价 免疫学
作者
Helen Melzer,Karin Baier,Franco Felici,Bernd-Ulrich Specht,G Wiedermann,Herwig Kollaritsch,Ursula Wiedermann,Michael DuchÃane
出处
期刊:Fems Immunology and Medical Microbiology [Oxford University Press]
卷期号:37 (2-3): 179-183 被引量:12
标识
DOI:10.1016/s0928-8244(03)00074-9
摘要

The protozoan parasite Entamoeba histolytica, which is responsible for intestinal amebiasis and amebic liver abscess, is causing significant morbidity and mortality worldwide. Proteophosphoglycans (PPGs, also known as lipophosphoglycans, LPGs, or lipopeptidophosphoglycans, LPPGs) are major surface components of E. histolytica. Passive immunization with a monoclonal antibody (EH5) directed against the PPGs protected severe combined immune-deficient mice from amebic liver abscess. The structure of the PPGs is very complex and only known in part. To find peptide mimics of E. histolytica PPG antigens, we had screened phage-displayed random peptide libraries with the antibody EH5. We identified various peptide mimics of E. histolytica PPGs, all sharing a consensus sequence Gly-Thr-His-Pro-X-Leu. Several of the phage clones induced a significant, specific IgG response against membrane antigens of E. histolytica after immunization of mice with whole phage particles. In the present work, in order to avoid the use of phage particles for immunization, we coupled two selected chemically synthesized peptides to keyhole limpet hemocyanin (KLH). The two KLH-conjugated peptides were immunogenic in mice and induced the production of high titers of anti-peptide antibodies, and one of the two peptides was also able to induce significant titers of antibodies against E. histolytica PPGs. Our results demonstrate that the KLH-conjugated peptides are able to mimic the EH5 epitope without the M13 phage sequences flanking the peptide inserts and independent of the structural framework of the phage.

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