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A Novel System for the Quantification of the ADCC Activity of Therapeutic Antibodies

机译:一种新型的治疗性抗体的ADCC活性定量系统

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摘要

Novel ADCC effector cells expressing the V-variant or F-variant of Fc γ RIIIa (CD16a) and firefly luciferase under the control of a chimeric promoter incorporating recognition sequences for the principal transcription factors involved in Fc γ RIIIa signal transduction, together with novel target cells overexpressing a constant high level of the specific antigen recognized by rituximab, trastuzumab, cetuximab, infliximab, adalimumab, or etanercept, confer improved sensitivity, specificity, and dynamic range in an ADCC assay relative to effector cells expressing a NFAT-regulated reporter gene and wild-type target cells. The effector cells also contain a normalization gene rendering ADCC assays independent of cell number or serum matrix effects. The novel effector and target cells in a frozen thaw-and-use format exhibit low vial-to-vial and lot-to-lot variation in their performance characteristics reflected by CVs of 10% or less. Homologous control target cells in which the specific target gene has been invalidated by genome editing providing an ideal control and a means of correcting for nonspecific effects were observed with certain samples of human serum. The novel effector cells and target cells expressing noncleavable membrane-bound TNF α have been used to quantify ADCC activity in serum from patients with Crohn's disease treated with infliximab and to relate ADCC activity to drug levels.
机译:在嵌合启动子的控制下,表达FcγRIIIa(CD16a)的V变异或F变异和萤火虫荧光素酶的新型ADCC效应细胞,并结合了涉及FcγRIIIa信号转导的主要转录因子的识别序列与利妥昔单抗,曲妥珠单抗,西妥昔单抗,英夫利昔单抗,阿达木单抗或依那西普识别的高水平恒定表达特定抗原的细胞相比,表达NFAT调控的报告基因和基因的效应细胞在ADCC分析中具有更高的敏感性,特异性和动态范围野生型靶细胞。效应细胞还包含归一化基因,可独立于细胞数量或血清基质效应进行ADCC分析。冷冻解冻和使用形式的新型效应子和靶细胞在小瓶到小瓶和批次之间的性能特征上表现出低的变异性,其CV反映在10%或以下。在某些人血清样品中观察到同源控制靶细胞,其中特定的靶基因已通过基因组编辑而失效,从而提供了理想的对照,并且纠正了非特异性作用的手段。表达不可切割的膜结合TNFα的新型效应细胞和靶细胞已用于量化英夫利昔单抗治疗的克罗恩病患者血清中的ADCC活性,并将ADCC活性与药物水平相关联。

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