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Tuning Relative Polypeptide Expression to Optimize Assembly Yield and Downstream Processing of Bispecific Antibodies

机译:调节相对多肽表达以优化双特异性抗体的装配产率和下游加工

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摘要

Bispecific antibodies (bsAbs) are often composed of several polypeptide chains that have to be expressed adequately to enable optimal assembly and yield of the bsAb. κλ bodies are a bispecific format with a native IgG structure, composed of two different light chains that pair with a common heavy chain. Introduction of non-optimal codons into the sequence of a particular polypeptide is an effective strategy for down modulating its expression. Here we applied this strategy but restricted the modification of the codon content to the constant domain of one light chain. This approach facilitates parallel optimization of several bsAbs by using the same modified constant domains. Partial sequence de-optimization reduced expression of the targeted polypeptide. Stable cell pools could be isolated displaying increased bispecific antibody titers as well as changes in the abundance of undesired by-products that require elimination during downstream processing. Thus, modulating the relative expression of polypeptides can have a significant impact on bsAb titer and product related impurities; which are important factors for large scale manufacturing for clinical supply.
机译:双特异性抗体(bsAbs)通常由几条多肽链组成,这些多肽链必须充分表达才能实现bsAb的最佳组装和产量。 κλ体是具有天然IgG结构的双特异性形式,由两条不同的轻链与一条共同的重链组成。将非最佳密码子引入特定多肽的序列是下调其表达的有效策略。在这里,我们应用了这种策略,但将密码子含量的修饰限制在一个轻链的恒定域。通过使用相同的修饰恒定域,该方法有助于并行优化几个bsAb。部分序列去最优化降低了靶多肽的表达。可以分离出稳定的细胞库,显示出增加的双特异性抗体滴度以及在下游加工过程中需要消除的不希望有的副产物的丰度变化。因此,调节多肽的相对表达可以对bsAb滴度和产物相关杂质产生重大影响。这是大规模生产临床供应的重要因素。

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