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Developing Peptide Mimotopes of Capsular Polysaccharides and Lipopolysaccharides Protective Antigens of Pathogenic Burkholderia Bacteria

机译:发育胶囊多糖和脂多糖的肽模拟物的致病毛刺细菌的脂多糖保护性抗原

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Burkholderia pseudomallei (BP) and Burkholderia mallei (BM) are two species of pathogenic Burkholderia bacteria. Our laboratory previously identified four monoclonal antibodies (MAbs) that reacted against Burkholderia capsular polysaccharides (PS) and lipopolysaccharides (LPS) and effectively protected against a lethal dose of BP/BM infections in mice. In this study, we used phage display panning against three different phage peptide libraries to select phage clones specifically recognized by each of the four protective MAbs. After sequencing a total of 179 candidate phage clones, we examined in detail six selected phage clones carrying different peptide inserts for the specificity of binding by the respective target MAbs. Chemically synthesized peptides corresponding to those displayed by the six phage clones were conjugated to keyhole limpet hemo-cyanin carrier protein and tested for their binding specificity to the respective protective MAbs. The study revealed that four of the six peptides, all derived from the library displaying dodecapeptides, functioned well as "mimotopes" of Burkholderia PS and LPS as demonstrated by a high degree of specific competition against the binding of three protective MAbs to BP and BM. Our results suggest that the four selected peptide mimics corresponding to PS/LPS protective antigens of BP and BM could potentially be developed into peptide vaccines against pathogenic Burkholderia bacteria.
机译:Burkholderia Pseudomallei(BP)和Burkholderia Mallei(BM)是两种致病伯克德利亚细菌。我们的实验室以前鉴定了四种单克隆抗体(MAB),其对Burkhowderia荚膜多糖(PS)和脂多糖(LPS)反应,并有效地保护小鼠中的致命剂量的BP / BM感染。在这项研究中,我们使用噬菌体展示淘选,针对三种不同的噬菌体肽文库来选择由四个保护性mAb中的每一个特异性识别的噬菌体克隆。测序总共179名候选噬菌体克隆后,我们将详细检查六种选定的噬菌体克隆,其具有各种靶MAb的结合的特异性的不同肽插入物。对应于六个噬菌体克隆所显示的肽的化学合成肽与孔孔颗粒血胞氰蛋白载体缀合,并测试其对各种保护性mAb的结合特异性。该研究表明,六种肽中的四种肽,均来自图书馆,其源自显示道肽肽,其作为Burkowneria PS和LPS的“Mimotopes”,如同高度的特定竞争对BP和BM的结合。我们的研究结果表明,对应于BP和BM的PS / LPS保护性抗原的四种选定的肽模拟物可能潜在地纳入肽疫苗,针对致病毛刺细菌。

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