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Dual-Color Bioluminescent Sensor Proteins for Therapeutic Drug Monitoring of Antitumor Antibodies

机译:双彩色生物发光传感器蛋白,用于抗肿瘤抗体治疗药物监测

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摘要

Monitoring the levels of therapeutic antibodies in individual patients would allow patient-specific dose optimization, with the potential for major therapeutic and financial benefits. Our group recently developed a new platform of bioluminescent sensor proteins (LUMABS; LUMinescent AntiBody Sensor) that allow antibody detection directly in blood plasma. In this study, we targeted four clinically important therapeutic antibodies, the Her2-receptor targeting trastuzumab, the anti-CD20 antibodies rituximab and obinutuzumab, and the EGFR-blocking cetuximab. A strong correlation was found between the affinity of the antibody binding peptide and sensor performance. LUMABS sensors with physiologically relevant affinities and decent sensor responses were obtained for trastuzumab and cetuximab using mimotope and meditope peptides, respectively, with affinities in the 10~(–7) M range. The lower affinity of the CD20-derived cyclic peptide employed in the anti-CD20 LUMABS sensor ( K _(d) = 10~(–5) M), translated in a LUMABS sensor with a strongly attenuated sensor response. The trastuzumab and cetuximab sensors were further characterized with respect to binding kinetics and their performance in undiluted blood plasma. For both antibodies, LUMABS-based detection directly in plasma compared well to the analytical performance of commercial ELISA kits. Besides identifying important design parameters for the development of new LUMABS sensors, this work demonstrates the potential of the LUMABS platform for point-of-care detection of therapeutic antibodies.
机译:监测个体患者的治疗性抗体水平将使患者特异性剂量优化,具有主要的治疗和财务效益的潜力。我们的团体最近开发了一种新的生物发光传感器蛋白(Lumabs;发光抗体传感器)的新平台,其允许直接血浆中的抗体检测。在这项研究中,我们针对四种临床上重要的治疗抗体,Her2-受体靶向Trastuzumab,抗CD20抗体Rituximab和ObInutuzumab,以及Egfl阻断的甲卓昔单抗。在抗体结合肽和传感器性能的亲和力之间发现了强的相关性。使用模拟物和蛋黄肽分别在10〜( - 7)M范围内的亲曲线和蛋白质蛋白,获得具有生理相关亲和力和体面传感器响应的Lumabs传感器和体面的传感器响应。 CD20衍生的环肽在抗CD20型亮度传感器(K _(d)= 10〜(-5)m)中的较低亲和力,在Lumabs传感器中翻译,具有牢固的传感器响应。相对于结合动力学和它们在未稀释的血浆中的性能方面进一步表征了曲妥珠单抗和西妥昔单抗传感器。对于两种抗体,直接在血浆中的基于洛米布的检测比较了商业ELISA试剂盒的分析性能。除了确定新的Lumabs传感器的开发的重要设计参数外,这项工作表明了Lumabs平台的潜力,用于治疗抗体的护理点检测。

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  • 来源
    《Analytical chemistry》 |2018年第5期|共8页
  • 作者单位

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

    Laboratory of Chemical Biology and Institute for Complex Molecular Systems (ICMS) Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 5600 MB Eindhoven The Netherlands;

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  • 正文语种 eng
  • 中图分类 分析化学;
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