首页> 外文期刊>Virology >Detection and characterization of functional T-cell epitopes on the structural proteins VP2, VP3, and VP4 of foot and mouth disease virus O1 campos.
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Detection and characterization of functional T-cell epitopes on the structural proteins VP2, VP3, and VP4 of foot and mouth disease virus O1 campos.

机译:检测和鉴定口蹄疫病毒O1营地的结构蛋白VP2,VP3和VP4上的功能性T细胞表位。

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Foot and mouth disease virus (FMDV) is the cause of a widespread infectious disease affecting cloven-hoofed animals. It is controlled by vaccination with immune-inactivated virus grown in tissue culture. However, peptide vaccines represent a safer alternative to the current virus-inactivated immunogens. Their design requires the identification and evaluation of the sequences recognized by T- and B-lymphocytes. Four structural proteins, VP1, VP2, VP3, and VP4, comprise the viral capsid of the FMDV, but only VP1 has been extensively studied regarding the existence of relevant T-cell epitopes. Here, we utilize a murine model to present a functional T-cell epitope mapping on the complete sequences of VP2, VP3, and VP4 of FMDV O1 Campos. We used two in vitro assays to describe 13 amino acid sequences, each one of them including at least one T-cell epitope. The in vivo T-cell helper function of these sequences was studied in an adoptive cell-transfer assay in mice. Immunization experiments with a fusion peptide containing one of the sequences characterized were also done comparing the helper activity of this sequence with other T-cell epitopes included in the major immunogenic region of VP1. Copyright 2000 Academic Press.
机译:口蹄疫病毒(FMDV)是影响偶蹄动物的广泛传染病的病因。通过接种在组织培养物中生长的免疫灭活病毒进行控制。但是,肽疫苗是目前病毒灭活免疫原的更安全替代品。他们的设计需要鉴定和评估T淋巴细胞和B淋巴细胞识别的序列。四个结构蛋白VP1,VP2,VP3和VP4组成了FMDV的病毒衣壳,但只有VP1被广泛研究了相关T细胞表位的存在。在这里,我们利用鼠模型在FMDV O1 Campos的VP2,VP3和VP4的完整序列上展示功能性T细胞表位。我们使用两种体外测定法描述了13个氨基酸序列,每个序列都包含至少一个T细胞表位。在小鼠的过继细胞转移试验中研究了这些序列的体内T细胞辅助功能。还比较了含有一个特征序列的融合肽进行的免疫实验,比较了该序列与VP1主要免疫原性区域中包含的其他T细胞表位的辅助活性。版权所有2000学术出版社。

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