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Arginine Modifications by Methylglyoxal: Discovery in a Recombinant Monoclonal Antibody and Contribution to Acidic Species

机译:甲基乙二醛精氨酸修饰:重组单克隆抗体中的发现和对酸性物种的贡献。

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摘要

Heterogeneity is common among protein therapeutics. For example, the so-called acidic species (charge variants) are typically observed when recombinant monoclonal antibodies (mAbs) are analyzed by weak-cation exchange chromatography (WCX). Several protein post-translational modifications have been established as contributors but still cannot completely account for all heterogeneity. As reported herein, an unexpected modification by methylglyoxal (MGO) was identified, for the first time, in a recombinant monoclonal antibody expressed in Chinese hamster ovary (CHO) cells. Modifications of arginine residues by methylglyoxal lead to two adducts (dihydroxyimidazolidine and hydroimidazolone) with increases of molecular weights of 72 and 54 Da, respectively. In addition, the modification by methylglyoxal causes the antibody to elute earlier in the weak cation exchange chromatogram. Consequently, the extent to which an antibody was modified at multiple sites corresponds to the degree of shift in elution time. Furthermore, cell culture parameters also affected the extent of modifications by methylglyoxal, a highly reactive metabolite that can be generated from glucose or lipids or other metabolic pathways. Our findings again highlight the impact that cell culture conditions can have on the product quality of recombinant protein pharmaceuticals.
机译:异质性在蛋白质治疗剂中很常见。例如,当通过弱阳离子交换色谱法(WCX)分析重组单克隆抗体(mAb)时,通常会观察到所谓的酸性物质(电荷变体)。已经确定了几种蛋白质翻译后修饰作为贡献者,但仍不能完全解释所有异质性。如本文所报道,在中国仓鼠卵巢(CHO)细胞中表达的重组单克隆抗体中首次鉴定出甲基乙二醛(MGO)的意外修饰。甲基乙二醛对精氨酸残基的修饰导致两个加合物(二羟基咪唑烷和氢咪唑啉酮)的分子量分别增加了72和54 Da。另外,甲基乙二醛的修饰导致抗体在弱阳离子交换色谱图中更早地洗脱。因此,抗体在多个位点被修饰的程度对应于洗脱时间的变化程度。此外,细胞培养参数还影响甲基乙二醛的修饰程度,甲基乙二醛是一种高反应性代谢物,可以从葡萄糖或脂质或其他代谢途径产生。我们的发现再次强调了细胞培养条件对重组蛋白药物产品质量的影响。

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