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Development of humanized monoclonal antibody by logical approach: Characterization, functional studies in vitro and immunogenicity studies in vivo in non-human primates

机译:通过逻辑方法开发人源化单克隆抗体:非人灵长类动物的表征,体外功能研究和体内免疫原性研究

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Monoclonal antibodies (mAbs) are widely used due to their exquisite specificity and once were hailed as the solution to cancer. However, when mouse mAbs are administered in humans, anti-antibody response (AAR) is frequently observed. Using humanized mAbs which are commonly developed by CDR-grafting method, the AAR is negligible, but loss of binding has also been consistently reported. Therefore, in an effort to produce humanized anti-C2 mAbs that retain binding properties but produce minimal AAR, humanized mAb has been developed by logical approach using IgBLAST. The purity and functionality of humanized mAb was confirmed bySodium dodecyl sulfate polyacrylamide gel electrophoresis(SDS-PAGE) and cell-based assays, respectively. Although the humanized mAb developed using logical approach had reduced AAR compared to mouse anti-C2 mAb inMacaca fascicularis, however the AAR was higher, compared to humanized mAb developed using deimmunization method. Hence, for the development of functional humanized mAbs with negligible AAR, it is recommended that amphipathic mouse residues, excluding those located in the CDR or Vernier zone, be chosen for humanization. However, humanization of every amphipathic mouse residues is unnecessary because with minimal judicious amino acid substitutions, an AAR response can be minimized without jeopardizing the immunoreactivity, hence making it ideal for use in human therapeutics.
机译:单克隆抗体(mAbs)由于其出色的特异性而被广泛使用,并且曾经被誉为癌症的解决方案。然而,当在人中施用小鼠mAb时,经常观察到抗抗体反应(AAR)。使用通常通过CDR嫁接方法开发的人源化mAb,AAR可以忽略不计,但也一直有报道说结合力下降。因此,在努力产生保留结合特性但产生最小的AAR的人源化抗C2 mAb的过程中,已经使用IgBLAST通过逻辑方法开发了人源化mAb。人源化mAb的纯度和功能分别通过十二烷基硫酸钠聚丙烯酰胺凝胶电泳(SDS-PAGE)和基于细胞的测定来确认。尽管在食蟹猕猴中使用逻辑方法开发的人源化mAb与小鼠抗C2 mAb相比具有降低的AAR,但是与使用脱免疫方法开发的人源化mAb相比,AAR更高。因此,为了开发具有可忽略的AAR的功能性人源化单克隆抗体,建议选择两亲性小鼠残基(不包括位于CDR或游标区中的残基)进行人源化。但是,不需要每一个两亲性小鼠残基的人源化,因为用最少的明智氨基酸取代,就可以在不损害免疫反应性的情况下将AAR反应减至最小,因此使其非常适合用于人体治疗。

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