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Macro- and Micro-Heterogeneity of Natural and Recombinant IgG Antibodies

机译:天然和重组IgG抗体的宏观和微观异质性

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摘要

Recombinant monoclonal antibodies (mAbs) intended for therapeutic usage are required to be thoroughly characterized, which has promoted an extensive effort towards the understanding of the structures and heterogeneity of this major class of molecules. Batch consistency and comparability are highly relevant to the successful pharmaceutical development of mAbs and related products. Small structural modifications that contribute to molecule variants (or proteoforms) differing in size, charge or hydrophobicity have been identified. These modifications may impact (or not) the stability, pharmacokinetics, and efficacy of mAbs. The presence of the same type of modifications as found in endogenous immunoglobulin G (IgG) can substantially lower the safety risks of mAbs. The knowledge of modifications is also critical to the ranking of critical quality attributes (CQAs) of the drug and define the Quality Target Product Profile (QTPP). This review provides a summary of the current understanding of post-translational and physico-chemical modifications identified in recombinant mAbs and endogenous IgGs at physiological conditions.
机译:需要对用于治疗用途的重组单克隆抗体(mAb)进行彻底表征,这已促进了广泛的工作,以了解这一主要分子的结构和异质性。批次一致性和可比性与单克隆抗体和相关产品的成功药物开发高度相关。已经鉴定出有助于大小,电荷或疏水性不同的分子变体(或蛋白形式)的小结构修饰。这些修饰可能会(或不影响)mAb的稳定性,药代动力学和功效。与内源性免疫球蛋白G(IgG)中发现的相同类型的修饰可以大大降低mAb的安全风险。修饰的知识对于药物的关键质量属性(CQA)的排名和定义质量目标产品资料(QTPP)也是至关重要的。这篇综述总结了目前对重组mAb和内源性IgG在生理条件下鉴定的翻译后和理化修饰的理解。

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