首页> 外文OA文献 >Evaluation of the Potency of Two Pyolysin-Derived Recombinant Proteins as Vaccine Candidates of Trueperella Pyogenes in a Mouse Model: Pyolysin Oligomerization and Structural Change Affect the Efficacy of Pyolysin-Based Vaccines
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Evaluation of the Potency of Two Pyolysin-Derived Recombinant Proteins as Vaccine Candidates of Trueperella Pyogenes in a Mouse Model: Pyolysin Oligomerization and Structural Change Affect the Efficacy of Pyolysin-Based Vaccines

机译:评估两种糊酶衍生的重组蛋白作为小鼠模型中Trueperella PoOgenes的疫苗候选的效力:臀蛋白寡聚化和结构变化影响了基于糊素的疫苗的疗效

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摘要

Trueperella pyogenes (T. pyogenes) is an important opportunistic pathogen in livestock and wild animals. However, only one commercial T. pyogenes vaccine is currently available, and its immunoprotective effect is not ideal. Pyolysin (PLO) is one of the important virulence factors expressed by T. pyogenes and one of the targets for the development of new T. pyogenes vaccines. In this study, we constructed two recombinant antigens, tPLOA1 (contains amino acids 1−110 and domain 4 of the PLO molecule) and tPLOA2 (contains amino acids 190−296 and domain 4 of the PLO molecule). Vaccines were prepared by mixing the two recombinant antigens with incomplete Freund's adjuvant or sheep red blood cell membrane and provided partial immune protection to immunized mice against the lethal challenge of T. pyogenes. Analysis of the PLO-specific IgG levels of immunized mice indicated that the antibody-inducing potency and immunoprotective efficacy of PLO-based vaccines are affected by the oligomerization and structural changes of PLO after binding to a cholesterol-containing membrane. In addition, the titer of anti-hemolysis antibodies is not a suitable indicator of the immunoprotective effect of these vaccines in PLO-based vaccine-immunized animals. The results provide new insights into the development of T. pyogenes vaccines.
机译:Trueperella pyogenes(T. pyogenes)是牲畜和野生动物的重要机会主义病原体。然而,目前只有一种商业T. pyogenes疫苗,其免疫保护作用并不理想。糊血素(PLO)是T. pyogenes表达的重要毒力因子之一,以及新的T. pyogenes疫苗的靶标的重要因素之一。在该研究中,我们构建了两种重组抗原,TPLOA1(含有PLO分子的氨基酸1-110和结构域4)和TPLOA2(含有PLO分子的氨基酸190-296和结构域4)。通过将两种重组抗原与不完全的弗氏佐剂或绵羊红细胞膜混合并为免疫小鼠提供部分免疫保护来制备疫苗,以抵御T. pyogenes的致命攻击。免疫小鼠PLO特异性IgG水平的分析表明,PLO基疫苗的抗体诱导效力和免疫保护效应受到在含胆固醇膜结合后PLO的寡聚化和结构变化的影响。此外,抗溶血抗体的滴度不是这些疫苗在基于PLO基疫苗免疫动物中的免疫保护作用的合适指示剂。结果为T. pyogenes疫苗的发展提供了新的见解。

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