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首页> 外文期刊>Biotechnology and Bioengineering >Culture temperature modulates half antibody and aggregate formation in a Chinese hamster ovary cell line expressing a bispecific antibody
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Culture temperature modulates half antibody and aggregate formation in a Chinese hamster ovary cell line expressing a bispecific antibody

机译:培养温调节表达双特异性抗体的中国仓鼠卵巢细胞系中的半抗体和聚集体形成

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摘要

Therapeutic bispecific antibodies are formed by assembly of multichain polypeptides. In general, a bispecific antibody has two different light chains and two different heavy chains that fold and correctly pair via engineered interchain interactions. Because of some incorrect assembly, product-related impurities can be prevalent (e.g., half molecules, mispaired light chains, homodimers), requiring its removal during subsequent purification. In this study, we investigated the modulation of impurity levels in a stable Chinese hamster ovary cell line X expressing a bispecific antibody A formed by two light chains (LC1 and LC2) and two heavy chains (HC1 and HC2) that assembled intracellularly into a heterodimer (LC1-HC1 + LC2-HC2) via engineered charged residues. Cell line X exhibited the best volumetric productivity, growth, and viability in culture compared with other clones but also showed higher levels of half antibody species (10%); therefore, to minimize process yield loss, better understanding, and control of impurity formation was pursued. We found this cell line decreased half antibody levels from 16% to 1% when temperature changed from 36 degrees C to 32.5 degrees C or 31.5 degrees C. However, lower temperature also increased high-molecular-weight (HMW) species from 4% to 12%. To determine the impurity species composition, we characterized enriched fractions with half antibody or HMW. Intact mass spectrometry analysis revealed half antibody was LC2-HC2, whereas HMW was a mixture with similar to 50% as LC1-HC1 homodimer. Results suggested LC2-HC2 was easily folded and could be secreted as half antibody, especially at 36 degrees C. On the contrary, LC1-HC1 was more susceptible to misfold or aggregate, a phenomenon more acute for cell line X at lower culture temperature because of 60% increased LC1 and HC1 messenger RNA levels. Although temperature modulation was cell line X-specific, the propensity of LC2-HC2 to form half antibodies and LC1-HC1 to aggregate a
机译:治疗性双特异性抗体是通过组装络合物的多肽而形成的。通常,双特异性抗体具有两种不同的轻链和两种不同的重链,通过工程间隔相互作用折叠并正确配对。由于组件一些不正确,产品相关的杂质可以普遍(例如,半分子,错误的光链,偶发二聚体),需要在随后的纯化期间去除。在这项研究中,我们研究了表达由两个轻链(LC1和LC2)形成的双特异性抗体A的稳定的中国仓鼠卵巢细胞系X中的杂质水平的调节和两种重链(HC1和HCl和HC 2),该抗体(LC1和LC2)和将细胞内组装成异二聚体(LC1-HC1 + LC2-HC2)通过工程用带电残余物。细胞系X与其他克隆相比,培养的最佳体积生产力,生长和活力表现出,但也显示出较高水平的半抗体物种(& 10%);因此,追求最小化过程产量损失,更好的理解和对杂质形成的控制。当温度从36摄氏度变为31.5℃或31.5℃时,我们发现这种细胞系从16%降低了16%至1%的抗体水平。然而,较低的温度也增加了4%的高分子量(HMW)物种。 12%。为了确定杂质物种组合物,我们用半抗体或HMW表征富集的级分。完整的质谱分析显示出半抗体是LC2-HC 2,而HMW是与LC1-HC1同型二聚体相似的混合物。结果表明LC2-HC2易于折叠,并且可以分泌为半抗体,特别是在36℃下分泌。相反,LC1-HC1更容易被误用或聚集体,对细胞系X较低的培养温度急性的现象,因为LC1和HC1信使RNA水平增加60%。虽然温度调节是细胞系X特异性的,但LC2-HC2的倾向形成半抗体和LC1-HC1聚集a

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