首页> 外文期刊>Scandinavian journal of immunology. >Synthesis and immunological activity of a branched peptide carrying the T-cell epitope of gp43, the major exocellular antigen of Paracoccidioides brasiliensis.
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Synthesis and immunological activity of a branched peptide carrying the T-cell epitope of gp43, the major exocellular antigen of Paracoccidioides brasiliensis.

机译:携带gp43 T细胞表位的分支肽的合成和免疫活性,gp43是巴西副球菌的主要胞外抗原。

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摘要

The 43 kDa glycoprotein (gp43) of Paracoccidioides brasiliensis is the major diagnostic antigen of paracoccidioidomycosis (PCM), a prevalent fungal infection in South America. A 15-mer sequence from gp43, denominated P10, induced T-CD4+ T helper 1 cellular immune responses in mice of three different haplotypes and protected against intratracheal challenge by a virulent isolate of P. brasiliensis. In an attempt to improve delivery of P10, a promiscuous antigen also presented by human leucocyte antigen-DR alleles, aiming at immunotherapy, we synthesized a multiple antigen peptide with the protective T-cell epitope expressed in a tetravalent 13-mer analog of P10 (M10). M10 induced specific lymph node cell proliferation in mice preimmunized with peptides in complete Freund's adjuvant (CFA). In addition, M10 immunization without CFA significantly protected intratracheally infected mice. We conclude that M10 is a candidate for an anti-PCM vaccine. In this report we describe: (1) the synthesis of M10; (2) theinduction of M10-elicited T-cell response and (3) in vivo protection of mice immunized with M10 and challenged by a virulent strain of P. brasiliensis.
机译:巴西副球菌的43 kDa糖蛋白(gp43)是副球菌病(PCM)的主要诊断抗原,这是南美一种常见的真菌感染。来自gp43的15-mer序列(命名为P10)在三种不同单倍型小鼠中诱导T-CD4 + T辅助1细胞免疫应答,并受到巴西乳杆菌的强毒分离物的保护,免受气管内攻击。为了改善P10(人类白细胞抗原-DR等位基因也提供的一种混杂抗原)的递送,旨在进行免疫治疗,我们合成了一种多抗原肽,具有在P10的四价13-mer类似物中表达的保护性T细胞表位( M10)。 M10在完全弗氏佐剂(CFA)中用肽预免疫的小鼠中诱导特异性淋巴结细胞增殖。此外,无CFA的M10免疫可显着保护气管内感染的小鼠。我们得出结论,M10是抗PCM疫苗的候选药物。在本报告中,我们描述:(1)M10的合成; (2)诱导M10诱导的T细胞应答和(3)体内保护受M10免疫并受到巴西假单胞菌强毒株攻击的小鼠。

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