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Functional Analysis of Neutralizing Antibodies against Clostridium perfringens Epsilon-Toxin▿

机译:抗产气荚膜梭菌Epsilon毒素中和抗体的功能分析

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摘要

The Clostridium perfringens epsilon-toxin causes a severe, often fatal illness (enterotoxemia) characterized by cardiac, pulmonary, kidney, and brain edema. In this study, we examined the activities of two neutralizing monoclonal antibodies against the C. perfringens epsilon-toxin. Both antibodies inhibited epsilon-toxin cytotoxicity towards cultured MDCK cells and inhibited the ability of the toxin to form pores in the plasma membranes of cells, as shown by staining cells with the membrane-impermeant dye 7-aminoactinomycin D. Using an antibody competition enzyme-linked immunosorbent assay (ELISA), a peptide array, and analysis of mutant toxins, we mapped the epitope recognized by one of the neutralizing monoclonal antibodies to amino acids 134 to 145. The antibody competition ELISA and analysis of mutant toxins suggest that the second neutralizing monoclonal antibody also recognizes an epitope in close proximity to this region. The region comprised of amino acids 134 to 145 overlaps an amphipathic loop corresponding to the putative membrane insertion domain of the toxin. Identifying the epitopes recognized by these neutralizing antibodies constitutes an important first step in the development of therapeutic agents that could be used to counter the effects of the epsilon-toxin.
机译:产气荚膜梭状芽胞杆菌的ε-毒素会导致严重,通常是致命的疾病(肠毒素血症),其特征是心脏,肺,肾和脑水肿。在这项研究中,我们检查了两种针对产气荚膜梭菌ε-毒素的中和单克隆抗体的活性。两种抗体均抑制了对培养的MDCK细胞的ε毒素的细胞毒性,并抑制了毒素在细胞质膜中形成孔的能力,如用不透膜的染料7-氨基放线菌素D对细胞染色所示。连锁免疫吸附测定(ELISA),肽阵列和突变毒素的分析,我们将被一种中和性单克隆抗体识别的表位定位在134至145位氨基酸上。抗体竞争ELISA和突变毒素的分析表明,第二种中和单克隆抗体还识别紧邻该区域的表位。由氨基酸134至145组成的区域与对应于毒素的推定膜插入结构域的两亲环重叠。鉴定被这些中和抗体识别的表位是开发可用于对抗ε-毒素作用的治疗剂的重要的第一步。

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