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Construction, expression and binding specificity of bispecific CD3 × VEGFR-2 and CD3 × NCAM antibodies in the single chain and diabody format

机译:双特异性和双抗体形式的双特异性CD3×VEGFR-2和CD3×NCAM抗体的构建,表达和结合特异性

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Bispecific antibodies are recombinant proteins with novel immunological properties and therapeutic potential. Recombinant protein quality and activity of several bispecific antibodies comprising different variable domain combinations with respect to the parental monospecific single chain fragments (scFv) were evaluated after expression in bacteria or mammalian cells. The parental scFv proteins humanized anti-NCAM scFv, murine anti-VEGFR-2 scFv, murine and humanized anti-CD3 scFv, respectively, could successfully be expressed in E. coli, whereas the murine anti-NCAM scFv version could not be reliably detected. Bispecific CD3 × VEGFR-2 and CD3 × NCAM anti-bodies were expressed in the bispecific single chain and the single chain diabody format. However, the diabody derived from the murine anti-NCAM scFv could not efficiently be expressed in E. coli or in mammalian cells. Significant binding of the CD3 × NCAM single chain diabody comprising the humanized version of anti-CD3 and humanized version of anti-NCAM was efficient to both antigens. Nevertheless, binding of the bispecific single chain version to the NCAM antigen was inefficient in comparison to CD3 binding. In conclusion, the data could indicate that the result of scFv expression in bacteria may be predictive for the chances of success for functional expression of more complex bispecific derivatives.
机译:双特异性抗体是具有新型免疫学性质和治疗潜力的重组蛋白。在细菌或哺乳动物细胞中表达后,评估相对于亲本单特异性单链片段(scFv)包含不同可变域组合的几种双特异性抗体的重组蛋白质量和活性。人源化抗NCAM scFv,鼠源抗VEGFR-2 scFv,鼠源和人源化抗CD3 scFv的亲本scFv蛋白可以分别在大肠杆菌中成功表达,但不能可靠地检测到鼠源抗NCAM scFv版本。双特异性CD3×VEGFR-2和CD3×NCAM抗体以双特异性单链和双链双抗体形式表达。但是,源自鼠抗NCAM scFv的双抗体不能在大肠杆菌或哺乳动物细胞中有效表达。包含人源化抗CD3版和人源化抗NCAM版的CD3×NCAM单链双抗体对两种抗原均有效结合。然而,与CD3结合相比,双特异性单链形式与NCAM抗原的结合效率低下。总之,数据可能表明细菌中scFv表达的结果可能是更复杂的双特异性衍生物功能表达成功的机会的预测。

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