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针对澳大利亚杀人蝎(Androctonus australis Hector)毒素II的单克隆抗体:表位特异性和中和能力的进一步表征

Monoclonal antibodies to toxin II from the scorpion Androctonus australis Hector: further characterization of epitope specificities and neutralizing capacities.

作者信息

Yahi N, Devaux C, Mansuelle P, Defendini M L, Granier C

机构信息

CNRS URA 1455, Laboratoire de Biochimie, Faculté de Médecine Secteur Nord, Marseille, France.

出版信息

Toxicon. 1992 Jul;30(7):723-31. doi: 10.1016/0041-0101(92)90006-q.

Abstract

The epitope specificities of two previously prepared monoclonal antibodies (mAb) to the toxin II from Androctonus australis Hector were characterized. Neither mAb 4C1 nor mAb 3C5 was able to recognize any of the 58 overlapping synthetic heptapeptides which cover the whole sequence of toxin II. Thus, both mAbs probably recognize conformation-dependent epitopes at the surface of the toxin. Experiments were designed to check whether or not the two mAbs, or their Fab fragments, were able to bind simultaneously to the toxin. The results indicated that the epitopes recognized by the two antibodies are probably close together at the surface of the toxin, thus preventing the simultaneous binding of both mAbs to a single toxin molecule. Given the proximity of the two epitopes and the fact that mAb 4C1 is known to be a neutralizing antibody, the capacity of mAb 3C5 to inhibit the toxic effects of the toxin was re-evaluated in C57BL/6 mice. A clear, but weak, neutralizing effect was found, consistent with the low affinity binding of the mAb in the proximity of a neutralizing site of the toxin.

摘要

对之前制备的两种针对澳大利亚红背蜘蛛(Androctonus australis Hector)毒素II的单克隆抗体(mAb)的表位特异性进行了表征。单克隆抗体4C1和单克隆抗体3C5均无法识别覆盖毒素II整个序列的58个重叠合成七肽中的任何一个。因此,这两种单克隆抗体可能识别毒素表面依赖构象的表位。设计实验以检查这两种单克隆抗体或其Fab片段是否能够同时结合毒素。结果表明,两种抗体识别的表位在毒素表面可能彼此靠近,从而阻止了两种单克隆抗体同时结合到单个毒素分子上。鉴于这两个表位的接近性以及已知单克隆抗体4C1是一种中和抗体,在C57BL/6小鼠中重新评估了单克隆抗体3C5抑制毒素毒性作用的能力。发现了明显但微弱的中和作用,这与单克隆抗体在毒素中和位点附近的低亲和力结合一致。

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