首页> 外文期刊>Analytical Biochemistry: An International Journal of Analytical and Preparative Methods >Characterization of intact antibody-drug conjugates from plasma/serum in vivo by affinity capture capillary liquid chromatography-mass spectrometry
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Characterization of intact antibody-drug conjugates from plasma/serum in vivo by affinity capture capillary liquid chromatography-mass spectrometry

机译:亲和捕获毛细管液相色谱-质谱法从体内血浆/血清中鉴定完整的抗体-药物偶联物

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摘要

Antibody-drug conjugates (ADCs) are designed to facilitate the targeted delivery of cytotoxic drugs to improve their tumor fighting effects and minimize systemic toxicity. However, efficacy and safety can potentially be compromised due to the release of conjugated drugs from the ADC with time while in circulation, resulting in changes in the drug-to-antibody ratio (DAR). Current understanding of this process is limited because existing methods such as immunoassays fail to distinguish ADCs with different DARs. Here we demonstrate a novel method with bead-based affinity capture and capillary liquid chromatography-mass spectrometry to allow direct measurement of drug release by quantifying DAR distributions of the ADC in plasma/serum. This method successfully identified individual intact conjugated antibody species produced due to drug loss from ADCs (e.g., an engineered site-specific anti-MUC16 THIOMAB-drug conjugate) and measured the corresponding DAR distributions in vitro and in vivo. Information obtained can provide insights into the mechanisms involved in drug loss and help to optimize ADC therapeutics. Other potential applications of the method may include characterization of posttranslational modifications, protein adducts, and immunogenicity.
机译:抗体-药物偶联物(ADC)旨在促进细胞毒性药物的靶向递送,以改善其抗肿瘤作用并使全身毒性最小化。但是,由于结合物随着时间的流逝从ADC释放,因此可能会损害功效和安全性,从而导致药物与抗体比率(DAR)发生变化。由于对现有方法(例如免疫分析)无法区分具有不同DAR的ADC,因此目前对该过程的了解受到限制。在这里,我们展示了一种基于珠粒的亲和捕获和毛细管液相色谱-质谱联用的新方法,通过量化血浆/血清中ADC的DAR分布,可以直接测量药物释放。该方法成功鉴定了由于ADC的药物流失而产生的单个完整的缀合抗体种类(例如,工程改造的位点特异性抗MUC16 THIOMAB-药物缀合物),并在体外和体内测量了相应的DAR分布。所获得的信息可以提供有关药物损失所涉及机制的见解,并有助于优化ADC治疗方法。该方法的其他潜在应用可能包括翻译后修饰,蛋白质加合物和免疫原性的表征。

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