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Boosting ADCC and CDC activity by Fc engineering and evaluation of antibody effector functions

机译:通过Fc工程增强ADCC和CDC活性并评估抗体效应子功能

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摘要

In recent years, therapy with monoclonal antibodies has become standard of care in various clinical applications. Despite obvious clinical activity, not all patients respond and benefit from this generally well tolerated treatment option. Therefore, rational optimization of antibody therapy represents a major area of interest in translational research. Animal models and clinical data suggested important roles of Fc-mediated effector mechanisms such as antibody dependent cell-mediated cytotoxicity (ADCC) or complement dependent cytotoxicity (CDC) in antibody therapy. These novel insights into the mechanisms of action mediated by monoclonal antibodies inspired the development of different engineering approaches to enhance/optimize antibodies' effector functions. Fc-engineering approaches by altering the Fc-bound glycosylation profile or by exchanging amino acids in the protein backbone have been intensively studied. Here, advanced and emerging technologies in Fc-engineering resulting in altered ADCC and CDC activity are summarized and experimental strategies to evaluate antibodies' effector functions are discussed.
机译:近年来,单克隆抗体疗法已成为各种临床应用中的护理标准。尽管有明显的临床活动,但并非所有患者都能对此总体耐受性良好的治疗方案做出反应并从中受益。因此,抗体疗法的合理优化代表了转化研究的主要兴趣领域。动物模型和临床数据表明,Fc介导的效应子机制(例如抗体依赖性细胞介导的细胞毒性(ADCC)或补体依赖性细胞毒性(CDC))在抗体治疗中具有重要作用。这些对单克隆抗体介导的作用机理的新颖见解激发了开发各种工程方法以增强/优化抗体效应子功能的灵感。通过改变Fc结合的糖基化谱或通过交换蛋白质主链中的氨基酸的Fc工程方法已被深入研究。在这里,总结了导致ADCC和CDC活性改变的Fc工程领域的先进技术,并讨论了评估抗体效应子功能的实验策略。

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