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首页> 外文期刊>Journal of Immunological Methods >Rheumatoid factor interference in immunogenicity assays for human monoclonal antibody therapeutics.
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Rheumatoid factor interference in immunogenicity assays for human monoclonal antibody therapeutics.

机译:类风湿因子干扰素对人单克隆抗体治疗剂的免疫原性测定。

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Rheumatoid factors (RFs) are endogenous human antibodies that bind to human gamma globulins. RFs demonstrate preferential binding to aggregated gamma globulins and are involved in the clearing mechanism of immune complexes. Immunoassays designed to measure human anti-human antibodies (HAHA) after administration of monoclonal antibody therapeutics are thus vulnerable to interference from RFs. When using a sensitive electrochemiluminescent (ECL) bridging immunoassay, samples from subjects with rheumatoid arthritis demonstrated much higher baseline reactivity than healthy subjects. Interference was found to be dependent on the aggregation state of the therapeutic antibody that had been conjugated with the detection reagent (ruthenium). Size exclusion high performance liquid chromatography (SE-HPLC) demonstrated that of the total integrated peaks, as little as 0.55% high molecular weight aggregates (>600kDa) were sufficient to cause increased reactivity. Stability studies of the ruthenium and biotin conjugated therapeutic antibody indicated that storage time, temperature and buffer formulation were critical in maintaining the integrity of the reagents. Through careful SE-HPLC monitoring we were able to choose appropriate storage and buffer conditions which led to a reduction in the false reactivity rate in therapeutic-naive serum from a rheumatoid arthritis population.
机译:类风湿因子(RF)是与人γ球蛋白结合的内源性人抗体。 RFs显示出对聚集的γ球蛋白的优先结合,并参与了免疫复合物的清除机制。因此,设计用于在施用单克隆抗体治疗剂后测量人抗人抗体(HAHA)的免疫测定法容易受到RF的干扰。当使用灵敏的电化学发光(ECL)桥接免疫测定法时,类风湿性关节炎受试者的样本显示出比健康受试者高得多的基线反应性。发现干扰取决于已与检测试剂(钌)偶联的治疗性抗体的聚集状态。尺寸排阻高效液相色谱(SE-HPLC)表明,在总积分峰中,低至0.55%的高分子量聚集体(> 600kDa)足以引起反应性的提高。钌和生物素缀合的治疗性抗体的稳定性研究表明,储存时间,温度和缓冲液配方对于维持试剂的完整性至关重要。通过仔细的SE-HPLC监测,我们能够选择合适的储存条件和缓冲条件,从而降低类风湿关节炎人群中未经治疗的血清中的假反应率。

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